US9561178B2 - Cyclosporin compositions - Google Patents

Cyclosporin compositions Download PDF

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US9561178B2
US9561178B2 US11/781,095 US78109507A US9561178B2 US 9561178 B2 US9561178 B2 US 9561178B2 US 78109507 A US78109507 A US 78109507A US 9561178 B2 US9561178 B2 US 9561178B2
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composition
drop
cyclosporin
another embodiment
provides
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US20080039378A1 (en
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Richard S. Graham
Walter L. Tien
Mayssa Attar
Rhett Schiffman
Aileen Morgan
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Saint Regis Mohawk Tribe
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Allergan Inc
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Priority to US11/858,200 priority patent/US20080146497A1/en
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Assigned to ALLERGAN, INC. reassignment ALLERGAN, INC. ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: GRAHAM, RICHARD S., SCHIFFMAN, RHETT, MORGAN, AILEEN, ATTAR, MAYSSA, TIEN, WALTER L.
Priority to US12/035,698 priority patent/US20080207495A1/en
Priority to US15/425,836 priority patent/US20170143792A1/en
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Priority to US17/064,988 priority patent/US20210169971A1/en
Priority to US17/663,188 priority patent/US20220409693A1/en
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K38/00Medicinal preparations containing peptides
    • A61K38/04Peptides having up to 20 amino acids in a fully defined sequence; Derivatives thereof
    • A61K38/12Cyclic peptides, e.g. bacitracins; Polymyxins; Gramicidins S, C; Tyrocidins A, B or C
    • A61K38/13Cyclosporins
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0048Eye, e.g. artificial tears
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/08Solutions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P27/00Drugs for disorders of the senses
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P27/00Drugs for disorders of the senses
    • A61P27/02Ophthalmic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P27/00Drugs for disorders of the senses
    • A61P27/02Ophthalmic agents
    • A61P27/04Artificial tears; Irrigation solutions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/02Inorganic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/08Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
    • A61K47/10Alcohols; Phenols; Salts thereof, e.g. glycerol; Polyethylene glycols [PEG]; Poloxamers; PEG/POE alkyl ethers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/26Carbohydrates, e.g. sugar alcohols, amino sugars, nucleic acids, mono-, di- or oligo-saccharides; Derivatives thereof, e.g. polysorbates, sorbitan fatty acid esters or glycyrrhizin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/30Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
    • A61K47/32Macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. carbomers, poly(meth)acrylates, or polyvinyl pyrrolidone
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/44Oils, fats or waxes according to two or more groups of A61K47/02-A61K47/42; Natural or modified natural oils, fats or waxes, e.g. castor oil, polyethoxylated castor oil, montan wax, lignite, shellac, rosin, beeswax or lanolin

Definitions

  • FIG. 1 Mean ( ⁇ SD) cornea cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
  • FIG. 2 Mean ( ⁇ SD) conjunctiva cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
  • FIG. 3 Mean ( ⁇ SD) sclera cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
  • FIG. 4 Mean ( ⁇ SD) eyelid margin cyclosporine A (concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
  • FIG. 5 Mean ( ⁇ SD) nasolacrimal duct cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
  • composition comprising cyclosporin A at a concentration of from about 0.0001% (w/v) to less than about 0.05% (w/v) is disclosed herein.
  • compositions of cyclosporin A at a concentration of less than about 0.05% (w/v) can be prepared that will be therapeutically effective.
  • compositions disclosed herein are administered to an eye of a mammal in need thereof to enhance or restore lacrimal gland tearing.
  • compositions disclosed herein are administered to an eye of a mammal in need thereof to increase tear production in a tear-deficient eye.
  • compositions disclosed herein are administered to an eye of a mammal in need thereof to treat keratoconjunctivitis sicca.
  • compositions disclosed herein are administered to an eye of a mammal in need thereof to treat dry eye disease.
  • Cyclosporin A is a cyclic peptide with immunosuppressive properties having the structure shown above. It is also known by other names including cyclosporine, cyclosporine A, ciclosporin, and ciclosporin A.
  • One embodiment is a method of treating dry eye disease comprising topically administering to a mammal in need thereof a composition comprising cyclosporin A at a concentration of from 0.0001% (w/v) to less than about 0.05% (w/v).
  • the treatment generally comprises administering 10-50 ⁇ L drops of the compositions disclosed herein topically to the eye or eyes of the mammal or human. Determination of the number of drops administered per day to the person or mammal to provide effective relief is within the skill of the ordinary artisan.
  • the composition is administered from 1 to 4 times per day.
  • the composition is administered twice a day.
  • composition is administered only once a day.
  • treat refers to the use of a compound, composition, therapeutically active agent, or drug in the diagnosis, cure, mitigation, treatment, prevention of disease or other undesirable condition, or to affect the structure or any function of the body of man or other animals.
  • the concentration of cyclosporin A is less than about 0.05%. This is intended to mean that the concentration is lower than the concentration in the commercially available 0.05% cyclosporin A emulsion known as Restasis®.
  • the concentration of cyclosporin A is from about 0.005% (w/v) to about 0.04% (w/v).
  • the concentration of cyclosporin A is from about 0.02% (w/v) to about 0.04% (w/v).
  • the concentration of cyclosporine A is about 0.005% (w/v).
  • the concentration of cyclosporine A is about 0.015% (w/v).
  • the concentration of cyclosporine A is about 0.02% (w/v).
  • the concentration of cyclosporine A is about 0.03% (w/v).
  • the concentration of cyclosporine A is about 0.04% (w/v).
  • a liquid which is ophthalmically acceptable is formulated such that it can be administered topically to the eye.
  • the comfort should be maximized as much as practicable, although sometimes formulation considerations (e.g. drug stability, bioavailability, etc.) may necessitate less than optimal comfort.
  • the liquid should be formulated such that the liquid is tolerable to the patient for topical ophthalmic use.
  • an ophthalmically acceptable liquid should either be packaged for single use, or contain a preservative to prevent contamination over multiple uses.
  • solutions or medicaments are often prepared using a physiological saline solution as a major vehicle. Ophthalmic solutions are often maintained at a comfortable pH with an appropriate buffer system.
  • the formulations may also contain conventional, pharmaceutically acceptable preservatives, stabilizers and surfactants.
  • buffers include, but are not limited to, acetate buffers, citrate buffers, phosphate buffers and borate buffers. Acids or bases may be used to adjust the pH of these formulations as needed.
  • the composition contains a preservative.
  • Preservatives that may be used in the pharmaceutical compositions disclosed herein include, but are not limited to, cationic preservatives such as
  • the composition contains a surfactant.
  • a surfactant may be used for assisting in dissolving an excipient or an active agent, dispersing a solid or liquid in a composition, enhancing wetting, modifying drop size, or a number of other purposes.
  • Useful surfactants include, but are not limited to surfactants of the following classes: alcohols; amine oxides; block polymers; carboxylated alcohol or alkylphenol ethoxylates; carboxylic acids/fatty acids; ethoxylated alcohols; ethoxylated alkylphenols; ethoxylated aryl phenols; ethoxylated fatty acids; ethoxylated; fatty esters or oils (animal & veg.); fatty esters; fatty acid methyl ester ethoxylates; glycerol esters; glycol esters; lanolin-based derivatives; lecithin and lecithin derivatives; lignin and lignin derivatives; methyl esters; monoglycerides
  • ethoxylate surfactants are useful.
  • An ethoxylate surfactants is one that comprises the moiety —O(CH 2 CH 2 O) n —OH, wherein n is at least about 1.
  • n is from about 1 to about 10,000.
  • n is from 1 to about 1000.
  • n is from about 1 to about 500.
  • Some ethoxylates contain one ethoxylate moiety. In other words, there is a single ethoxylate chain on each molecule.
  • surfactants with one ethoxylate moiety include, but are not limited to:
  • Ethoxylated alcohols wherein the alcohol has a single hydroxyl unit; alkylphenol ethoxylates; ethoxylated fatty acids; fatty acid methyl ester ethoxylates; polyethylene glycols; and the like.
  • Ethoxylates may comprise more than one ethoxylate moiety. In other words, there may be ethoxylate moieties attached to several different parts of the molecule. Examples include, but are not limited to: block polymers; ethoxylated oils; sorbitan derivatives; sucrose and glucose ethoxylates; and the like.
  • Block Polymers These are polymers with the structure A-B-A′, wherein A and A′ are polyethylene chains of 1 or more ethylene units, and B is a polypropylene chain of one or more propylene units. Generally, but not necessarily, A and A′ are approximately the same length. In one embodiment, A and A′ contain from about 2 to about 200 ethylene units. In another embodiment, A and A′ contain from about 5 to about 100 ethylene units. In another embodiment, A and A′ contain about 7 to about 15 ethylene units. In another embodiment, A and A′ contain about 7, about 8, or about 12 ethylene units. In another embodiment, B contains from about 25 to about 100 propylene units. In another embodiment, B contains from about 30 to about 55 propylene units.
  • B contains about 30, about 34, or about 54 propylene units.
  • the molecular weight is from about 1000 to about 20000. In another embodiment, the molecular weight is from about 2000 to about 10000. In another embodiment, the molecular weight is about 2500, about 3000, about 3800, or about 8400. These include but are not limited to: Poloxalene: wherein A has about 12 ethylene oxide units, B has about 34 propylene oxide units, A′ has about 12 ethylene oxide units, and the average molecular weight is about 3000.
  • Poloxamer 182 wherein A has about 8 ethylene oxide units, B has about 30 propylene oxide units, A′ has about 8 ethylene oxide units, and the average molecular weight is about 2500
  • Poloxamer 188 wherein A has about 75 ethylene oxide units, B has about 30 propylene oxide units, A′ has about 75 ethylene oxide units, and the average molecular weight is about 8400.
  • Poloxamer 331 wherein A has about 7 ethylene oxide units, B has about 54 propylene oxide units, A′ has about 7 ethylene oxide units, and the average molecular weight is about 3800; Ethoxylated Alcohols These include but are not limited to: Ethoxylates of linear alcohols having from about 6 to about 20 carbon atoms.
  • the linear alcohol has from about 10 to about 16 carbon atoms.
  • n is from about 1 to about 100.
  • n is from about 1 to about 50.
  • n is from about 5 to about 50 ethylene oxide units.
  • n is from about 1 to about 20 ethylene oxide units.
  • n is from about 30 to about 50 ethylene oxide units.
  • Ethoxylated Alkylphenols These are alkylphenols that are ethoxylated, i.e. the phenolic OH is replaced with an ethoxylate moiety. These include but are not limited to: octylphenol ethoxylate, i.e. CH 17 Ph(OCH 2 CH 2 O) n H.
  • nonylphenol ethoxylate i.e. CH 19 Ph (OCH 2 CH 2 O) n H. alkyphenols of the above formula wherein n is from about 1 to about 100. alkyphenols of the above formula wherein n is from about 1 to about 50. alkyphenols of the above formula wherein n is from about 9 to about 15.
  • Octyl Phenol 1.5 Mole Ethoxylate (i.e. n is an average of about 1.5); Octyl Phenol 5 Mole Ethoxylate; Octyl Phenol 7 Mole Ethoxylate; Octyl Phenol 9 Mole Ethoxylate; Octyl Phenol 12 Mole Ethoxylate; Octyl Phenol 40 Mole Ethoxylate; Nonyl Phenol 1.5 Mole Ethoxylate; Nonyl Phenol 4 Mole Ethoxylate; Nonyl Phenol 6 Mole Ethoxylate; Nonyl Phenol 9 Mole Ethoxylate; Nonyl Phenol 10 Mole Ethoxylate; Nonyl Phenol 10.5 Mole Ethoxylate; Nonyl Phenol 12 Mole Ethoxylate; Nonyl Phenol 15 Mole Ethoxylate; Nonyl Phenol 15 Mole Ethoxylate; Nonyl Phenol 30 Mole Ethoxylate;
  • Ethylene oxide may also react with a fatty acid ester with a formula RCO 2 R′ to form RCO 2 (CH 2 CH 2 O) n R′.
  • RCO 2 R′ a formula RCO 2 R′
  • surfactants having the formula RCO 2 (CH 2 CH 2 O) n R′, where RCO 2 H is a fatty acid and R′ is alkyl having from 1 to 6 carbons are contemplated.
  • One embodiment is a fatty acid methyl ester ethoxylate, wherein R′ is methyl.
  • RCO 2 H is Lauric Acid; a 14 carbon fatty acid such as myristic acid; a 16 carbon fatty acid such as palmitic and palmitoleic acid; an 18 carbon fatty acids such as stearic acid, oleic acid, linoleic acid, ⁇ -linolenic acid, and ⁇ -linolenic acid; a 20 carbon fatty acids such as eicosapentaenoic acid; a 22 carbon fatty acids such as arachidic acid; or a 24 carbon fatty acids such as lignoceric acid and nervonic acid.
  • Polyethylene Glycols are ethoxylates that are unsubstituted, or terminated with oxygen on both ends, i.e. HO(CH 2 CH 2 O) n H,
  • polysorbate 80 has an oleate cap as shown in the structure below.
  • POE w+x+y+z sorbitan mono (or di- or tri-) fatty acid.
  • Polysorbate 80 is POE (2O) sorbitan monooleate.
  • the number in parenthesis is the total number of ethylene oxide units on the molecule, and the ending is the number of acid caps and the capping acid.
  • Sorbitan derivatives wherein the total number of ethylene oxide units is from 3 to 30; Sorbitan derivatives wherein the total number of ethylene oxide units is 4, 5, or 20; Sorbitan derivatives wherein the capping acid is laurate, palmitate, stearate, or oleate;
  • the sorbitan derivative may be a POE sorbitan monolaurate; a POE sorbitan dilaurate; a POE sorbitan trilaurate; a POE sorbitan monopalmitate; a POE sorbitan dipalmitate; a POE sorbitan tripalmitate; a POE sorbitan monostearate; a POE sorbitan distearate; a POE sorbitan tristearate; a POE sorbitan monooleate; a POE sorbitan dioleate; or a POE sorbitan trioleate; Specific examples include: POE (20)
  • sucrose and glucose esters are simply ethoxylated, but do not have a capping carboxylic acid.
  • Other sucrose and glucose esters may be ethoxylated and capped with an alkyl group formed by reaction with an alcohol.
  • Other sucrose and glucose esters may be esters or ethers of the sugars with hydrophobic chains and have ethoxylates substituted in other positions on the sugar.
  • Various useful vehicles may be used in the ophthalmic preparations disclosed herein. These vehicles include, but are not limited to, polyvinyl alcohol, povidone, hydroxypropyl methyl cellulose, poloxamers, carboxymethyl cellulose, hydroxyethyl cellulose, and acrylates (e.g. Pemulen®).
  • Tonicity adjustors may be added as needed or convenient. They include, but are not limited to, salts, particularly sodium chloride, potassium chloride, mannitol and glycerin, or any other suitable ophthalmically acceptable tonicity adjustor.
  • an ophthalmically acceptable antioxidant includes, but is not limited to, sodium metabisulfite, sodium thiosulfate, acetylcysteine, butylated hydroxyanisole and butylated hydroxytoluene.
  • excipient components which may be included in the ophthalmic preparations are chelating agents.
  • a useful chelating agent is edetate disodium, although other chelating agents may also be used in place or in conjunction with it.
  • Compositions may be aqueous solutions or emulsions, or some other acceptable liquid form.
  • one or more oils will be used to form the emulsion, and in some instances one or more surfactants will be required.
  • Suitable oils include, but are not limited to anise oil, castor oil, clove oil, cassia oil, cinnamon oil, almond oil, corn oil, arachis oil, cottonseed oil, safflower oil, maize oil, linseed oil, rapeseed oil, soybean oil, olive oil, caraway oil, rosemary oil, peanut oil, peppermint oil, sunflower oil, eucalyptus oil, sesame oil, and the like.
  • the composition is an aqueous solution.
  • the composition contains no ethanol.
  • the composition contains no hyauronic acid.
  • the composition contains no vitamin E TPGS.
  • the composition contains no cyclodextrin A.
  • the composition contains no cyclodextrin.
  • compositions P, A, B and C are prepared according to the following procedure.
  • Target pH is 7.5+/ ⁇ 0.1.
  • the sterile filtrate can then be aseptically dispensed into multidose dropper bottles suitable for ophthalmic purpose.
  • the finished product should be tested for cyclosporine assay, pH, osmolality, viscosity, Purite, sterility, and antimicrobial effectiveness.
  • the finished product should be store at room temperature and protected from light.
  • D and E were prepared by standard methods known in the art.
  • F was prepared as described above for A-C except that Pemulen TR-2 was substituted for carboxymethylcellulose sodium, and the addition of the citrate and borate buffers were omitted.
  • compositions disclosed and used herein provide a therapeutically effective amount of cyclosporin A to a mammal.
  • concentrations of cyclosporin A in the compositions may be significantly lower than those normally associated with a therapeutically effective concentration.
  • one commercial preparation, marketed as Restasis® by Allergan, Inc. is a 0.05% cyclosporin A castor oil emulsion.
  • Other compositions currently in development have concentrations of 0.1% or higher.
  • the composition provides more cyclosporin A to the cornea of a person than Composition AA.
  • composition provides more cyclosporin A to the cornea of a person than Composition BB.
  • composition provides more cyclosporin A to the cornea of a person than Composition CC.
  • the composition provides more cyclosporin A to the cornea of a person than Composition DD.
  • composition provides more cyclosporin A to the cornea of a person than Composition EE.
  • composition provides more cyclosporin A to the cornea of a person than Composition FF.
  • the composition provides more cyclosporin A to the cornea of a person than Composition GG.
  • composition provides more cyclosporin A to the cornea of a person than Composition HH.
  • composition provides more cyclosporin A to the cornea of a person than Composition II.
  • composition JJ provides more cyclosporin A to the cornea of a person than Composition JJ.
  • composition provides more cyclosporin A to the cornea of a person than Composition KK.
  • composition provides more cyclosporin A to the cornea of a person than Composition LL.
  • composition provides more cyclosporin A to the cornea of a person than Composition MM.
  • the composition provides more cyclosporin A to the conjunctiva of a person than Composition AA.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition BB.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition CC.
  • the composition provides more cyclosporin A to the conjunctiva of a person than Composition DD.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition EE.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition FF.
  • the composition provides more cyclosporin A to the conjunctiva of a person than Composition GG.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition HH.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition II.
  • composition JJ provides more cyclosporin A to the conjunctiva of a person than Composition JJ.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition KK.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition LL.
  • composition provides more cyclosporin A to the conjunctiva of a person than Composition MM.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 500 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 1000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 1400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 17000 ng of cyclosporin A per gram of cornea of said rabbit over a period of 24 hours after said topical administration.
  • said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 ⁇ L drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit as determined by:
  • said composition to each eye of a New Zealand rabbit provides at least about 30000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
  • said composition to each eye of a New Zealand rabbit provides at least about 45000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
  • composition to each eye of a New Zealand rabbit provides at least about 95000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
  • said composition to each eye of a New Zealand rabbit provides at least about 155000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the conjunctivas of said rabbit at least about 6000 ng of cyclosporin A per gram of conjunctiva of said rabbit over a period of 24 hours after said topical administration.
  • said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 ⁇ L drop of said composition to each eye of a New Zealand rabbit provides at least about 6000 ng of cyclosporin A per gram of conjunctiva to the conjunctivas of said rabbit as determined by:
  • said composition to each eye of a New Zealand rabbit provides at least about 5000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
  • said composition to each eye of a New Zealand rabbit provides at least about 7000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
  • said composition to each eye of a New Zealand rabbit provides at least about 10000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
  • said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
  • the blood level of cyclosporin A is less than 0.1 mg/mL for a person for whom the composition has been administered twice a day topically to both eyes in 35 microliter drops for twelve months.
  • compositions D, E, and F as described above, were used for these experiments.
  • mice Female New Zealand White rabbits weighing 1.8 to 2.6 kg were purchased from Charles River (St. Constant, Quebec, Canada). A permanent ear tag was used to identify animals.
  • the animals were provided Certified Hi-Fiber Rabbit Diet. Diet certification and analysis were provided by the vendor. No analysis outside those provided by the manufacturer was performed. Drinking water that was purified by a reverse osmosis process was offered ad libitum. Water was periodically analyzed for any contaminants that may interfere with the conduct of this study.
  • Animals were euthanized via injection of at least 1 mL of sodium pentobarbital into a marginal ear vein.
  • a ketamine/xylazine cocktail 87 mg/mL ketamine, 13 mg/mL xylazine
  • Ocular samples were collected from both eyes, blotted dry where applicable, weighed and placed in separate, appropriately labeled, silanized vials, at the time of necropsy. Both eyes were rinsed with LENS PLUS® in order to clear residual surface formulation remaining on the ocular surface.
  • the entire cornea was removed from each eye; weight recorded, placed into separate screw-cap glass 13 ⁇ 100 silanized test tubes and immediately placed on ice. Samples were stored at or below ⁇ 15° C. until bioanalysis.
  • the sclera was removed from each eye; weight recorded, placed into separate screw-cap glass 13 ⁇ 100 silanized test tubes and immediately placed on ice. Samples were stored at or below ⁇ 15° C. until bioanalysis.
  • Tissue containing the nasolacrimal duct associated with each eye was removed; weight recorded, placed into screw-cap glass 13 ⁇ 100 silanized test tubes and immediately placed on ice. Samples were stored at or below ⁇ 15° C. until bioanalysis.
  • Blood and ocular tissue samples were stored at or below ⁇ 15° C. until bioanalysis.
  • Ocular tissue and blood concentrations were quantified using the following method.
  • Ocular tissue samples were extracted by soaking over night with 2.0 mL methanol at 4° C. This was followed by a second soak with 2.0 mL methanol and shaking for approximately one hour at room temperature. An aliquot of 1 mL from a total of 4 mL organic extract was removed (all 4 mL were analyzed for lacrimal gland samples), and internal standard added (20 ⁇ L of 500 ng/mL of CsG). The methanolic extract was evaporated to dryness and reconstituted with 200 ⁇ L of 2 mM ammonium acetate/0.4% formic acid in 50:50 acetonitrile:water for LC MS/MS analysis. The bioanalytical procedure for analysis of blood samples involved addition of internal standard, CsG (10 ⁇ L of 500 ng/mL) to 0.5 mL aliquots of K3 EDTA-treated rabbit blood.
  • CsG 10 ⁇ L of 500 ng/mL
  • the precursor-product ion pairs used in MRM analysis were: 1203 (MH) + ⁇ 425.5 for CsA and m/z 1217 (MH) + ⁇ 425.5 for IS(Cyclosporin G).
  • the total analysis time was 5 min, with retention times of CsA and CsG at approximately 1.82 and 1.86 minutes, respectively.
  • Thermo Electron WatsonTM Philadelphia, Pa.
  • Microsoft® Excel Microsoft® Excel (Redmond, Wash.) were used for pharmacokinetic calculations.
  • the pharmacokinetic parameters listed below were calculated using a known non-compartmental approach (see Tang-Lui, et. al. Pharmaceutical Research , Vol 5, No. 4, 1988, 238-241).
  • the pharmacokinetic data was described using descriptive statistics such as mean and standard deviation whenever possible.
  • Area under the concentration-time profile (AUC) values were reported as a composite AUC and whenever possible, ⁇ standard error of the mean (SEM).
  • PK Parameter Description C max (ng/mL) or Maximum observed concentration (ng/g) T max (hr) Time corresponding to maximum observed concentration AUC 0-t (ng ⁇ hr/g) Area under concentration time curve from time zero to the last quantifiable time point using the random method for non-sequential sampling t 1/2 (hr) Half-life MRT (hr) Mean residence time Values below the Limit of Quantitation and Number Rounding
  • the mean concentrations and pharmacokinetic parameters are summarized in Tables 3 and 4.
  • the concentration-time profiles of cyclosporine A in cornea following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 1 .
  • cyclosporine A was rapidly absorbed into the cornea with a peak corneal concentration (C max ) of 4050 ⁇ 1220 ng/g, occurring 0.500 hours post-dose.
  • C max corneal concentration
  • the area under the concentration-time curve (AUC 0-t ) value through the last quantifiable time point was 163000 ⁇ 7000 ng ⁇ hr/g and the AUC 0-24 value was 59000 ng ⁇ hr/g.
  • the terminal half-life (t 1/2 ) was 41.3 hours and the mean residence time (MRT) was 50.3 hours.
  • cyclosporine A was absorbed into the cornea with C max value of 1100 ⁇ 190 ng/g, occurring 2.00 hours post-dose.
  • the AUC 0-t value was 76200 ⁇ 3300 ng ⁇ hr/g and the AUC 0-24 value was 22100 ng ⁇ hr/g.
  • the terminal t 1/2 was 41.7 hours and the MRT was 56.5 hours.
  • cyclosporine A was absorbed into the cornea with a C max value of 536 ⁇ 138 ng/g, occurring 6.00 hours post-dose.
  • the AUC 0-t value was 29300 ⁇ 2000 ng ⁇ hr/g and the AUC 0-24 value was 9450 ng ⁇ hr/g.
  • the terminal t 1/2 was 49.8 hours and the MRT was 61.6 hours.
  • composition F Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the conjunctiva with a C max value of 4460 ⁇ 650 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 18100 ⁇ 800 ng ⁇ hr/g and the AUC 0-24 value was 17100 ng ⁇ hr/g.
  • the terminal t 1/2 was 11.3 hours and the MRT was 7.37 hours.
  • composition E Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the conjunctiva with a C max value of 2560 ⁇ 1070 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 11600 ⁇ 700 ng ⁇ hr/g.
  • the terminal t 1/2 was 5.57 hours and the MRT was 5.93 hours.
  • cyclosporine A was rapidly absorbed into the conjunctiva with a C max value of 694 ⁇ 410 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 5290 ⁇ 480 ng ⁇ hr/g.
  • the terminal t 1/2 was 4.55 hours and the MRT was 6.07 hours.
  • composition F Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the sclera with a C max value of 545 ⁇ 98 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 6110 ⁇ 260 ng ⁇ hr/g and the AUC 0-24 value was 3900 ng ⁇ hr/g.
  • the terminal t 1/2 was 29.7 hours and the MRT was 25.3 hours.
  • composition E Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the sclera with a C max value of 136 ⁇ 43 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 2840 ⁇ 150 ng ⁇ hr/g and the AUC 0-24 value was 1560 ng ⁇ hr/g.
  • the terminal t 1/2 was 24.8 hours and the MRT was 26.7 hours.
  • cyclosporine A was absorbed into the sclera with a C max value of 53.0 ⁇ 10.9 ng/g, occurring 6.00 hours post-dose.
  • the AUC 0-t value was 1040 ⁇ 50 ng ⁇ hr/g and the AUC 0-24 value was 792 ng ⁇ hr/g.
  • the terminal t 1/2 was 18.7 hours and the MRT was 23.8 hours.
  • composition F Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the eyelid margin with a C max value of 3120 ⁇ 1040 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 38300 ⁇ 5300 ng ⁇ hr/g and the AUC 0-24 value was 19900 ng ⁇ hr/g.
  • the terminal t 1/2 was 42.5 hours and the MRT was 40.5 hours.
  • composition E Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the eyelid margin with a C max value of 2020 ⁇ 980 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 42200 ⁇ 10800 ng ⁇ hr/g and the AUC 0-24 value was 17600 ng ⁇ hr/g.
  • the terminal t 1/2 was 38.1 hours and the MRT was 38.4 hours.
  • cyclosporine A was absorbed into the eyelid margin with a C max value of 2450 ⁇ 970 ng/g, occurring 2.00 hours post-dose.
  • the AUC 0-t value was 27700 ⁇ 3300 ng ⁇ hr/g and the AUC 0-24 value was 18000 ng ⁇ hr/g.
  • the terminal t 1/2 was 24.4 hours and the MRT was 21.9 hours.
  • composition F Following a single bilateral ocular instillation of Composition F, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a C max value of 195 ⁇ 201 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 2190 ⁇ 350 ng ⁇ hr/g and the AUC 0-12 value was 478 ⁇ 86 ng ⁇ hr/g.
  • the MRT was 17.6 hours.
  • composition E Following a single bilateral ocular instillation of Composition E, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a C max value of 74.4 ⁇ 20.9 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 1190 ⁇ 210 ng ⁇ hr/g and the AUC 0-12 value was 465 ⁇ 106 ng ⁇ hr/g.
  • the MRT was 24.7 hours.
  • composition D Following a single bilateral ocular instillation of Composition D, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a C max value of 72.0 ⁇ 91.7 ng/g, occurring 0.500 hours post-dose.
  • the AUC 0-t value was 279 ⁇ 39 ng ⁇ hr/g.
  • the MRT was 12.1 hours.
  • cyclosporine A was detected at 0.5 and 2 hours post-dose in the blood at concentrations of 2.21 ⁇ 0.33 ng/mL and 0.463 ⁇ 0.021 ng/mL, respectively. Cyclosporine A levels were below the limit of quantitation at all subsequent time points.
  • cyclosporine A was detected at 0.5 hours post-dose in the blood at a concentration of 0.441 ⁇ 0.126 ng/mL. Cyclosporine A levels were below the limit of quantitation at all subsequent time points.
  • Composition F Administration of Composition F to rabbits generally delivered the highest levels of cyclosporine A to ocular tissues, on average a 5-fold increase in area under the concentration-time profile (AUC) was observed when compared to Composition D.
  • Administration of Composition E to rabbits resulted on average in a 2-fold increase in AUC when compared to Composition D.
  • the pharmacokinetic profile observed following Composition D administration to New Zealand White rabbits in this study was in good agreement with previously reported data.
  • the terminal half-life and mean residence time observed were greatest for Composition F, followed by the Composition E, followed by Composition D.
  • AUC values were reported to the last quantifiable time point, in addition to AUC through 24 hours for cornea, conjunctiva, sclera and eyelid margin and AUC through 12 hours for nasolacrimal duct to make an assessment over the same interval as to the drug levels achieved following once a day dosing.
  • the trends observed when comparing AUC 0-t values were consistent with the trends observed when comparing AUC 0-24 or AUC 0-12 .
  • compositions below were prepared in an analogous manner to compositions D, E, and F.
  • Formulations Composition G Composition H Composition Aqueous Aqueous D Ingredients Solution Solution Emulsion Cyclosporine A 0.020 0.030 0.050 Purite 0.01% 0.01% 0.0% (100 ppm) (100 ppm) (0 ppm) Polysorbate 80 1.0 1.0 1.0 1.0 Glycerin 1.0 1.0 2.2 Mannitol 0.5 0.5 N/A Sodium 0.5 0.5 N/A Carboxymethylcellulose (CMC) - 7LFPH Sodium Citrate 0.4 0.4 N/A Dihydrate Boric Acid 0.25 0.25 N/A Sodium Borate 0.41 0.41 N/A Decahydrate Potassium Chloride 0.14 0.14 N/A Castor Oil N/A N/A 1.25 Pemulen TR-2 N/A N/A 0.05 Sodium Hydroxide N/A N/A pH 7.4 Purified Water QS QS N/A
  • Test Formulations G, H, and D Animal species/strain: Rabbit NZW Gender: Female Number: 2 rabbits/timepoint (2 rabbits blanks) Dosing Route: Topical ocular Dosing Regimen: Bilateral, QD(Aqueous)/BID (Composition D) - 5 days Dose Volume: 35 ⁇ L Time points: Day 1 and Day 5 - 0.5, 2, 6, 12, 24 hr post dose Assay Method: LC-MS/MS Analyte: Cyclosporine A Data Analysis: C max , AUC 0-24 , AUC dose normalized
  • Composition D Composition G
  • compositions are particularly contemplated for use as standards for comparison for characterization of the compositions disclosed herein.
  • compositions are intended to mean those identical to those disclosed in Kanai et. al., Transplantation Proceedings , Vol 21, No 1 (February), 1989: 3150-3152, which is incorporated by reference herein:
  • composition is intended to mean those identical to that disclosed in Cheeks et. al., Current Eye Research , Vol 11, No 7 (1992), 641-649, which is incorporated by reference herein:
  • composition is intended to mean that identical that disclosed in Tamilvanan, Stp Pharma Sci November-December; 11(6):421-426, which is incorporated by reference herein, except that the concentration of cyclosporin A is different.
  • compositions are intended to mean those identical to Samples C-E disclosed in U.S. Pat. No. 5,051,402 (column 7). The entire disclosure is incorporated herein by reference.
  • composition is intended to mean that identical that disclosed in Abdulrizak, Stp Pharma Sci November-December; 11(6):427-432, which is incorporated by reference herein, except that the concentration of cyclosporin A is different.
  • composition is intended to mean that identical to that disclosed in Kuwano Mitsuaki et al. Pharm Res 2002 August; 19(1):108-111.
  • composition is intended to mean that disclosed in Example 2 of U.S. Pat. No. 5,951,971, incorporated herein by reference.
  • composition provides more cyclosporin A than Composition AA provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
  • composition provides more cyclosporin A than Composition BB provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
  • composition provides more cyclosporin A than Composition CC provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
  • composition provides more cyclosporin A than Composition DD provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
  • composition provides more cyclosporin A than Composition EE provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
  • composition provides more cyclosporin A than Composition FF provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
  • composition provides more cyclosporin A than Composition GG provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
  • composition provides more cyclosporin A than Composition HH provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
  • composition provides more cyclosporin A than Composition II provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
  • composition JJ provides more cyclosporin A than Composition JJ provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
  • composition provides more cyclosporin A than Composition KK provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
  • composition provides more cyclosporin A than Composition LL provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
  • composition provides more cyclosporin A than Composition MM provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
  • composition provides more cyclosporin A than Composition AA provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
  • composition provides more cyclosporin A than Composition BB provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
  • composition provides more cyclosporin A than Composition CC provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
  • composition provides more cyclosporin A than Composition DD provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
  • composition provides more cyclosporin A than Composition EE provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
  • composition provides more cyclosporin A than Composition FF provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
  • composition provides more cyclosporin A than Composition GG provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
  • composition provides more cyclosporin A than Composition HH provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
  • composition provides more cyclosporin A than Composition II provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
  • composition JJ provides more cyclosporin A than Composition JJ provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
  • composition provides more cyclosporin A than Composition KK provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
  • composition provides more cyclosporin A than Composition LL provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
  • composition provides more cyclosporin A than Composition MM provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
  • Comparison of two compositions in a person or animal can be carried out by, among other means, administering the claimed composition to one eye and the second composition to the second eye.
  • composition provides more cyclosporin A than Composition AA provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
  • composition provides more cyclosporin A than Composition BB provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
  • composition provides more cyclosporin A than Composition CC provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
  • composition provides more cyclosporin A than Composition DD provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
  • composition provides more cyclosporin A than Composition EE provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
  • composition provides more cyclosporin A than Composition FF provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
  • composition provides more cyclosporin A than Composition GG provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
  • composition provides more cyclosporin A than Composition HH provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
  • composition provides more cyclosporin A than Composition II provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
  • composition JJ provides more cyclosporin A than Composition JJ provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
  • composition provides more cyclosporin A than Composition KK provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
  • composition provides more cyclosporin A than Composition LL provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
  • composition provides more cyclosporin A than Composition MM provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
  • composition provides more cyclosporin A than Composition AA provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
  • composition provides more cyclosporin A than Composition BB provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
  • composition provides more cyclosporin A than Composition CC provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
  • composition provides more cyclosporin A than Composition DD provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
  • composition provides more cyclosporin A than Composition EE provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
  • composition provides more cyclosporin A than Composition FF provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
  • composition provides more cyclosporin A than Composition GG provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
  • composition provides more cyclosporin A than Composition HH provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
  • composition provides more cyclosporin A than Composition II provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
  • composition JJ provides more cyclosporin A than Composition JJ provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
  • composition provides more cyclosporin A than Composition KK provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
  • composition provides more cyclosporin A than Composition LL provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
  • composition provides more cyclosporin A than Composition MM provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 500 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 17000 ng of cyclosporin A per gram of cornea of said rabbit over a period of 24 hours after said topical administration.
  • topical administration of one 35 ⁇ L drop of said composition to each eye of a female New Zealand white rabbit provides to the conjunctivas of said rabbit at least about 3300 ng of cyclosporin A per gram of conjunctiva of said rabbit over a period of 24 hours after said topical administration.
  • said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 ⁇ L drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit as determined by:
  • said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 ⁇ L drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of conjunctiva to the conjunctivas of said rabbit as determined by:
  • compositions are suitable for use in other mammals other than rabbits, including humans.
  • any composition in the claims or elsewhere which is characterized by in vivo rabbit bioavailability testing is contemplated for use in a person or in another mammal. Defining a composition in terms of bioavailability in rabbits should not be construed to limit a method of treatment using the composition to use on rabbits, but treatment with the composition should be construed to include treatment on humans and other mammals.

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Abstract

Disclosed herein are therapeutic methods, compositions, and medicaments related to cyclosporine.

Description

RELATED APPLICATION
This application is based, and claims priority under 35 U.S.C. §120 to U.S. Provisional Application Ser. No. 60/820,239, filed Jul. 25, 2006; U.S. Provisional Application Ser. No. 60/829,796, filed Oct. 17, 2006; U.S. Provisional Application Ser. No. 60/829,808, filed Oct. 17, 2006; U.S. Provisional Application Ser. No. 60/883,525, filed Jan. 5, 2007; U.S. Provisional Application Ser. No. 60/916,352, filed May 7, 2007; and U.S. Provisional Application Ser. No. 60/869,459, filed Dec. 11, 2006; each of which is hereby incorporated by reference in their entirety.
BACKGROUND OF THE INVENTION
Abnormalities associated with the function of the lacrimal gland or with tearing often cause discomfort to mammals who suffer from these abnormalities.
BRIEF DESCRIPTION OF THE DRAWINGS
FIG. 1 Mean (±SD) cornea cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
FIG. 2 Mean (±SD) conjunctiva cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
FIG. 3 Mean (±SD) sclera cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
FIG. 4 Mean (±SD) eyelid margin cyclosporine A (concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
FIG. 5 Mean (±SD) nasolacrimal duct cyclosporine A concentrations (semi-log) following a single bilateral topical ocular instillation of one of three 0.05% cyclosporine A formulations to New Zealand White rabbits.
 DETAILED DESCRIPTION OF THE INVENTION
A composition comprising cyclosporin A at a concentration of from about 0.0001% (w/v) to less than about 0.05% (w/v) is disclosed herein.
We have surprisingly discovered that compositions of cyclosporin A at a concentration of less than about 0.05% (w/v) can be prepared that will be therapeutically effective.
In one embodiment, the compositions disclosed herein are administered to an eye of a mammal in need thereof to enhance or restore lacrimal gland tearing.
In another embodiment, the compositions disclosed herein are administered to an eye of a mammal in need thereof to increase tear production in a tear-deficient eye.
In another embodiment, the compositions disclosed herein are administered to an eye of a mammal in need thereof to treat keratoconjunctivitis sicca.
In another embodiment, the compositions disclosed herein are administered to an eye of a mammal in need thereof to treat dry eye disease.
Figure US09561178-20170207-C00001
Cyclosporin A is a cyclic peptide with immunosuppressive properties having the structure shown above. It is also known by other names including cyclosporine, cyclosporine A, ciclosporin, and ciclosporin A.
Treatment Methods
One embodiment is a method of treating dry eye disease comprising topically administering to a mammal in need thereof a composition comprising cyclosporin A at a concentration of from 0.0001% (w/v) to less than about 0.05% (w/v).
The treatment generally comprises administering 10-50 μL drops of the compositions disclosed herein topically to the eye or eyes of the mammal or human. Determination of the number of drops administered per day to the person or mammal to provide effective relief is within the skill of the ordinary artisan.
In one embodiment, the composition is administered from 1 to 4 times per day.
In another embodiment, the composition is administered twice a day.
In another embodiment, the composition is administered only once a day.
In another embodiment, less than 14% of patients suffer ocular burning when the composition is administered only once a day for a period of three months.
In another embodiment, less than 10% of patients suffer ocular burning when the composition is administered only once a day for a period of three months.
In another embodiment, less than 8% of patients suffer ocular burning when the composition is administered only once a day for a period of three months.
For the purposes of this disclosure, “treat,” “treating,” or “treatment” refer to the use of a compound, composition, therapeutically active agent, or drug in the diagnosis, cure, mitigation, treatment, prevention of disease or other undesirable condition, or to affect the structure or any function of the body of man or other animals.
Compositions
The concentration of cyclosporin A is less than about 0.05%. This is intended to mean that the concentration is lower than the concentration in the commercially available 0.05% cyclosporin A emulsion known as Restasis®.
In another embodiment, the concentration of cyclosporin A is from about 0.005% (w/v) to about 0.04% (w/v).
In another embodiment, the concentration of cyclosporin A is from about 0.02% (w/v) to about 0.04% (w/v).
In another embodiment, the concentration of cyclosporine A is about 0.005% (w/v).
In another embodiment, the concentration of cyclosporine A is about 0.015% (w/v).
In another embodiment, the concentration of cyclosporine A is about 0.02% (w/v).
In another embodiment, the concentration of cyclosporine A is about 0.03% (w/v).
In another embodiment, the concentration of cyclosporine A is about 0.04% (w/v).
A liquid which is ophthalmically acceptable is formulated such that it can be administered topically to the eye. The comfort should be maximized as much as practicable, although sometimes formulation considerations (e.g. drug stability, bioavailability, etc.) may necessitate less than optimal comfort. In the case that comfort cannot be maximized, the liquid should be formulated such that the liquid is tolerable to the patient for topical ophthalmic use. Additionally, an ophthalmically acceptable liquid should either be packaged for single use, or contain a preservative to prevent contamination over multiple uses.
For ophthalmic application, solutions or medicaments are often prepared using a physiological saline solution as a major vehicle. Ophthalmic solutions are often maintained at a comfortable pH with an appropriate buffer system. The formulations may also contain conventional, pharmaceutically acceptable preservatives, stabilizers and surfactants.
Various buffers and means for adjusting pH may be used so long as the resulting preparation is ophthalmically acceptable. Accordingly, buffers include, but are not limited to, acetate buffers, citrate buffers, phosphate buffers and borate buffers. Acids or bases may be used to adjust the pH of these formulations as needed.
In another embodiment, the composition contains a preservative.
Preservatives that may be used in the pharmaceutical compositions disclosed herein include, but are not limited to, cationic preservatives such as
    • quaternary ammonium compounds including benzalkonium chloride, polyquad, and the like;
    • guanidine-based preservatives including PHMB, chlorhexidine, and the like;
      chlorobutanol;
      mercury preservatives such as thimerosal, phenylmercuric acetate and phenylmercuric nitrate; and
      oxidizing preservatives such as stabilized oxychloro complexes (e.g. Purite®).
In another embodiment, the composition contains a surfactant.
A surfactant may be used for assisting in dissolving an excipient or an active agent, dispersing a solid or liquid in a composition, enhancing wetting, modifying drop size, or a number of other purposes. Useful surfactants include, but are not limited to surfactants of the following classes: alcohols; amine oxides; block polymers; carboxylated alcohol or alkylphenol ethoxylates; carboxylic acids/fatty acids; ethoxylated alcohols; ethoxylated alkylphenols; ethoxylated aryl phenols; ethoxylated fatty acids; ethoxylated; fatty esters or oils (animal & veg.); fatty esters; fatty acid methyl ester ethoxylates; glycerol esters; glycol esters; lanolin-based derivatives; lecithin and lecithin derivatives; lignin and lignin derivatives; methyl esters; monoglycerides and derivatives; polyethylene glycols; polymeric surfactants; propoxylated & ethoxylated fatty acids, alcohols, or alkyl phenols; protein-based surfactants; sarcosine derivatives; sorbitan derivatives; sucrose and glucose esters and derivatives.
In particular, ethoxylate surfactants are useful.
An ethoxylate surfactants is one that comprises the moiety —O(CH2CH2O)n—OH, wherein n is at least about 1.
In one embodiment n is from about 1 to about 10,000.
In another embodiment, n is from 1 to about 1000.
In another embodiment, n is from about 1 to about 500.
Some ethoxylates contain one ethoxylate moiety. In other words, there is a single ethoxylate chain on each molecule.
Examples of surfactants with one ethoxylate moiety, include, but are not limited to:
Ethoxylated alcohols wherein the alcohol has a single hydroxyl unit; alkylphenol ethoxylates; ethoxylated fatty acids; fatty acid methyl ester ethoxylates; polyethylene glycols; and the like.
Ethoxylates may comprise more than one ethoxylate moiety. In other words, there may be ethoxylate moieties attached to several different parts of the molecule. Examples include, but are not limited to: block polymers; ethoxylated oils; sorbitan derivatives; sucrose and glucose ethoxylates; and the like.
Block Polymers: These are polymers with the structure A-B-A′, wherein A and A′ are polyethylene chains of 1 or more ethylene units, and B is a polypropylene chain of one or more propylene units. Generally, but not necessarily, A and A′ are approximately the same length.
In one embodiment, A and A′ contain from about 2 to about 200 ethylene units.
In another embodiment, A and A′ contain from about 5 to about 100 ethylene units.
In another embodiment, A and A′ contain about 7 to about 15 ethylene units.
In another embodiment, A and A′ contain about 7, about 8, or about 12 ethylene units.
In another embodiment, B contains from about 25 to about 100 propylene units.
In another embodiment, B contains from about 30 to about 55 propylene units.
In another embodiment, B contains about 30, about 34, or about 54 propylene units.
In another embodiment, the molecular weight is from about 1000 to about 20000.
In another embodiment, the molecular weight is from about 2000 to about 10000.
In another embodiment, the molecular weight is about 2500, about 3000, about 3800, or about 8400.
These include but are not limited to:
Poloxalene: wherein A has about 12 ethylene oxide units, B has about 34 propylene oxide units, A′ has about 12 ethylene oxide units, and the average molecular weight is about 3000.
Poloxamer 182: wherein A has about 8 ethylene oxide units, B has about 30 propylene oxide units, A′ has about 8 ethylene oxide units, and the average molecular weight is about 2500
Poloxamer 188: wherein A has about 75 ethylene oxide units, B has about 30 propylene oxide units, A′ has about 75 ethylene oxide units, and the average molecular weight is about 8400.
Poloxamer 331: wherein A has about 7 ethylene oxide units, B has about 54 propylene oxide units, A′ has about 7 ethylene oxide units, and the average molecular weight is about 3800;
Ethoxylated Alcohols
These include but are not limited to:
Ethoxylates of linear alcohols having from about 6 to about 20 carbon atoms.
In one embodiment, the linear alcohol has from about 10 to about 16 carbon atoms.
In another embodiment, n is from about 1 to about 100.
In another embodiment, n is from about 1 to about 50.
In another embodiment, n is from about 5 to about 50 ethylene oxide units.
In another embodiment, n is from about 1 to about 20 ethylene oxide units.
In another embodiment, n is from about 30 to about 50 ethylene oxide units.
Ethoxylated Alkylphenols
These are alkylphenols that are ethoxylated, i.e. the phenolic OH is replaced with an ethoxylate moiety.
These include but are not limited to:
octylphenol ethoxylate, i.e. CH17Ph(OCH2CH2O)nH.
nonylphenol ethoxylate, i.e. CH19Ph (OCH2CH2O)nH.
alkyphenols of the above formula wherein n is from about 1 to about 100.
alkyphenols of the above formula wherein n is from about 1 to about 50.
alkyphenols of the above formula wherein n is from about 9 to about 15.
Octyl Phenol 1.5 Mole Ethoxylate (i.e. n is an average of about 1.5); Octyl Phenol 5 Mole Ethoxylate; Octyl Phenol 7 Mole Ethoxylate; Octyl Phenol 9 Mole Ethoxylate; Octyl Phenol 12 Mole Ethoxylate; Octyl Phenol 40 Mole Ethoxylate; Nonyl Phenol 1.5 Mole Ethoxylate; Nonyl Phenol 4 Mole Ethoxylate; Nonyl Phenol 6 Mole Ethoxylate; Nonyl Phenol 9 Mole Ethoxylate; Nonyl Phenol 10 Mole Ethoxylate; Nonyl Phenol 10.5 Mole Ethoxylate; Nonyl Phenol 12 Mole Ethoxylate; Nonyl Phenol 15 Mole Ethoxylate; Nonyl Phenol 15 Mole Ethoxylate; Nonyl Phenol 30 Mole Ethoxylate; and Nonyl Phenol 40 Mole Ethoxylate; Ethoxylated Fatty Acids,
These include but are not limited to:
ethoxylates which are esterified to form either:
    • monoesters, i.e. RCO2(CH2CH2O)nOH, where RCO2H is a fatty acid; or
    • diesters, i.e. RCO2(CH2CH2O)nC(═O)R.
      Fatty acids include, but are not limited to:
      Saturated fatty acids, which have no C═C moieties and include myristic acid, palmitic acid, stearic acid, arachidic acid, behenic acid, lignoceric acid.
      Unsaturated fatty acids, including the following:
    • monounsaturated fatty acids, which have one C═C group such as palmitoleic acid, oleic acid, and nervonic acid;
    • diunsaturated fatty acids, which have two C═C groups, such as linoleic acid;
    • triiunsaturated fatty acids, which have three C═C groups, such as α-linolenic acid and γ-linolenic acid;
    • tetraunsaturated fatty acids, which have four C═C groups, such as arachidonic acid; and
    • pentaunsaturated fatty acids, which have five C═C groups, such as eicosapentaenoic acid.
      The following may also be used:
      Lauric Acid; 14 carbon fatty acids such as myristic acid; 16 carbon fatty acids such as palmitic and palmitoleic acid; 18 carbon fatty acids such as stearic acid, oleic acid, linoleic acid, α-linolenic acid, and γ-linolenic acid; 20 carbon fatty acids such as eicosapentaenoic acid; 22 carbon fatty acids such as arachidic acid; and 24 carbon fatty acids such as lignoceric acid and nervonic acid.
      In one embodiment, n is from about 2 to about 100.
      In another embodiment, n is from about 5 to about 50.
      In another embodiment, n is from about 30 to 50.
      Ethoxylated Fatty Esters or Oils (Animal & Veg.).
      These are the products which result from reacting ethylene oxide with a fatty ester or an oil. When a fatty oil is used, the products is a mixture of ethoxylates of the fatty acids present in the oil, ethoxylates of glycerine, ethoxylates of mono and diglycerides, and the like.
      Specific examples include, but are not limited to:
      Ethoxylates of the following oils: Anise oil, Castor oil, Clove oil, Cassia oil, Cinnamon oil; Almond oil, Corn oil, Arachis oil, Cottonseed oil, Safflower oil, Maize oil, Linseed oil, Rapeseed oil, Soybean oil, Olive oil, Caraway oil, Rosemary oil, Peanut oil, Peppermint oil, Sunflower oil, Eucalyptus oil and Sesame oil; Coriander oil, Lavender oil, Citronella oil, Juniper oil, Lemon oil, Orange oil, Clary sage oil, Nutmeg oil, Tea tree oil, coconut oil, tallow oil, and lard;
      In one embodiment, from 1 to about 50 moles of ethylene oxide is used per mole of the oil triglyceride.
      In another embodiment, from about 30 to about 40 moles of ethylene oxide is used per mole of the oil triglyceride.
Ethylene oxide may also react with a fatty acid ester with a formula RCO2R′ to form RCO2(CH2CH2O)nR′. Thus, surfactants having the formula RCO2(CH2CH2O)nR′, where RCO2H is a fatty acid and R′ is alkyl having from 1 to 6 carbons are contemplated.
One embodiment is a fatty acid methyl ester ethoxylate, wherein R′ is methyl.
In another embodiment, RCO2H is Lauric Acid; a 14 carbon fatty acid such as myristic acid; a 16 carbon fatty acid such as palmitic and palmitoleic acid; an 18 carbon fatty acids such as stearic acid, oleic acid, linoleic acid, α-linolenic acid, and γ-linolenic acid; a 20 carbon fatty acids such as eicosapentaenoic acid; a 22 carbon fatty acids such as arachidic acid; or a 24 carbon fatty acids such as lignoceric acid and nervonic acid.
Polyethylene Glycols are ethoxylates that are unsubstituted, or terminated with oxygen on both ends, i.e. HO(CH2CH2O)nH,
Sorbitan Derivatives:
These are ethoxylated sorbates having a fatty acid capping one or more of the ethoxylated chains. For example, polysorbate 80 has an oleate cap as shown in the structure below.
Figure US09561178-20170207-C00002
These compounds are named as POE (w+x+y+z) sorbitan mono (or di- or tri-) fatty acid.
For example, Polysorbate 80 is POE (2O) sorbitan monooleate. Thus, the number in parenthesis is the total number of ethylene oxide units on the molecule, and the ending is the number of acid caps and the capping acid.
These include but are not limited to:
Sorbitan derivatives wherein the total number of ethylene oxide units is from 3 to 30;
Sorbitan derivatives wherein the total number of ethylene oxide units is 4, 5, or 20;
Sorbitan derivatives wherein the capping acid is laurate, palmitate, stearate, or oleate;
The sorbitan derivative may be a POE sorbitan monolaurate;
a POE sorbitan dilaurate;
a POE sorbitan trilaurate;
a POE sorbitan monopalmitate;
a POE sorbitan dipalmitate;
a POE sorbitan tripalmitate;
a POE sorbitan monostearate;
a POE sorbitan distearate;
a POE sorbitan tristearate;
a POE sorbitan monooleate;
a POE sorbitan dioleate;
or a POE sorbitan trioleate;
Specific examples include:
POE (20) sorbitan monolaurate; POE (4) sorbitan monolaurate; POE (20) sorbitan monopalmitate; POE (20) monostearate; POE (20) sorbitan monostearate; POE (4) sorbitan monostearate; POE (20) sorbitan tristearate; POE (20) sorbitan monoleate; POE (20) sorbitan 15 monoleate; POE (5) sorbitan 10 monoleate; POE (20) sorbitan trioleate; and
Sucrose and Glucose Esters and Derivatives:
Although there are a number of sucrose and glucose based surfactants, some sucrose and glucose esters and derivatives are similar to the sorbate derivatives described above. In other words, one, several, or all of the hydroxyl moieties of the sugar are ethoxylated, and one or more of the ethoxylate chains are capped with a carboxylic acid. Other sucrose and glucose esters are simply ethoxylated, but do not have a capping carboxylic acid. Other sucrose and glucose esters may be ethoxylated and capped with an alkyl group formed by reaction with an alcohol. Other sucrose and glucose esters may be esters or ethers of the sugars with hydrophobic chains and have ethoxylates substituted in other positions on the sugar.
Various useful vehicles may be used in the ophthalmic preparations disclosed herein. These vehicles include, but are not limited to, polyvinyl alcohol, povidone, hydroxypropyl methyl cellulose, poloxamers, carboxymethyl cellulose, hydroxyethyl cellulose, and acrylates (e.g. Pemulen®).
Tonicity adjustors may be added as needed or convenient. They include, but are not limited to, salts, particularly sodium chloride, potassium chloride, mannitol and glycerin, or any other suitable ophthalmically acceptable tonicity adjustor.
In a similar vein, an ophthalmically acceptable antioxidant includes, but is not limited to, sodium metabisulfite, sodium thiosulfate, acetylcysteine, butylated hydroxyanisole and butylated hydroxytoluene.
Other excipient components which may be included in the ophthalmic preparations are chelating agents. A useful chelating agent is edetate disodium, although other chelating agents may also be used in place or in conjunction with it.
Compositions may be aqueous solutions or emulsions, or some other acceptable liquid form. For an emulsion, one or more oils will be used to form the emulsion, and in some instances one or more surfactants will be required. Suitable oils include, but are not limited to anise oil, castor oil, clove oil, cassia oil, cinnamon oil, almond oil, corn oil, arachis oil, cottonseed oil, safflower oil, maize oil, linseed oil, rapeseed oil, soybean oil, olive oil, caraway oil, rosemary oil, peanut oil, peppermint oil, sunflower oil, eucalyptus oil, sesame oil, and the like.
In one embodiment, the composition is an aqueous solution.
In another embodiment, the composition contains no ethanol.
In another embodiment, the composition contains no hyauronic acid.
In another embodiment, the composition contains no vitamin E TPGS.
In another embodiment, the composition contains no cyclodextrin A.
In another embodiment, the composition contains no cyclodextrin.
Example 1
Percent
Ingredients Amount needed (g)
Ingredients (% w/v) for a 1 liter batch
Cyclosporine
0% for Placebo 0 grams for Placebo
(P) (P)
0.03% (A) 0.30 (A)
0.04% (B) 0.40 (B)
0.05% (C) 0.5 (C)
Carboxymethylcellulose 0.5 5.0
sodium
Polysorbate 80 1.0 10.0
Glycerin 1.0 10.0
Mannitol 0.5 5.0
Sodium Citrate 0.4 4.0
Dihydrate
Boric Acid 0.25 2.5
Sodium Borate 0.41 4.1
Decahydrate
Potassium Chloride 0.14 1.4
Purite 0.01 0.1
Purified Water q.s. to 100% q.s to 100%
Compositions P, A, B and C, are prepared according to the following procedure.
1. Measure Purified Water to about 90% of the batch size and place in an appropriate beaker or container.
2. Begin mixing the water with a strong mixer (Rotosolver) to obtain a strong vortex.
3. Add the pre-weighed carboxymethylcellulose sodium into the strong vortex. Continue strong mixing for at least 1 hour.
4. Slow mixer to a slow speed.
5. Add and dissolve the pre-weighed polysorbate 80.
6. Add and dissolve the pre-weighed glycerin.
7. Add and dissolve the pre-weighed mannitol.
8. Add and dissolve the pre-weighed sodium citrate dehydrate.
9. Add and dissolve the pre-weighed boric acid.
10. Add and dissolve the pre-weighed sodium borate decahydrate.
11. Add and dissolve the pre-weighed potassium chloride.
12. Check pH and adjust if necessary. Target pH is 7.5+/−0.1.
13. Add and dissolve the pre-weighed Purite.
14. Add sufficient quantity of Purified Water to attain the final batch volume. This will provide the finished placebo formulation (P).
Procedure for Either 0.03% (A), 0.04% (B), 0.05% (C)
15. Measure the exact amount of Placebo (9815×) needed to satisfy the batch size requirements and place in a media bottle that contains a magnetic stir bar.
16. Add and dissolve the pre-weighed cyclosporine. Stir at a slow speed to avoid foaming. It will usually take overnight mixing to completely dissolve the cyclosporine.
17. After overnight mixing is completed, pump the cyclosporine solution through a Millipore Milligard pre-filter and a Pall Suporlife sterilizing filter and collect the filtrate aseptically.
18. The sterile filtrate can then be aseptically dispensed into multidose dropper bottles suitable for ophthalmic purpose.
19. The finished product should be tested for cyclosporine assay, pH, osmolality, viscosity, Purite, sterility, and antimicrobial effectiveness.
20. The finished product should be store at room temperature and protected from light.
Example 2
The following formulations were prepared. D and E were prepared by standard methods known in the art. F was prepared as described above for A-C except that Pemulen TR-2 was substituted for carboxymethylcellulose sodium, and the addition of the citrate and borate buffers were omitted.
D E F
Emulsion Emulsion Solution
Cyclosporin A 0.05 0.05 0.05
Castor Oil 1.25 0.30 N/A
Polyoxyethylene N/A 0.30 N/A
40 Stearate, NF
Polysorbate 80 1.00 0.30 1.00
Glycerin 2.20 1.00 1.00
Mannitol N/A 2.00 2.00
Pemulen TR-2 0.05 0.10 0.10
Sodium Hydroxide pH pH pH
(1N) adjustment adjustment adjustment
Purified Water QS QS QS
pH pH = 7.4 7.39 7.35

Bioavailability
The compositions disclosed and used herein provide a therapeutically effective amount of cyclosporin A to a mammal. However, while not intending to limit the scope of the invention in any way, concentrations of cyclosporin A in the compositions may be significantly lower than those normally associated with a therapeutically effective concentration. For example, one commercial preparation, marketed as Restasis® by Allergan, Inc., is a 0.05% cyclosporin A castor oil emulsion. Other compositions currently in development have concentrations of 0.1% or higher.
Reported herein are pharmacokinetic data for in vivo experiments on rabbits. However, the rabbit experiments are believed to be useful models for bioavailability in other mammals including humans. Thus, although bioavailability parameters are disclosed and featured in the claims, they should not be construed as limiting the treatment to rabbits only, but the compositions characterized and defined by bioavailability in rabbits are also contemplated for use in treatment in other mammals, particularly humans.
In one embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition AA.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition BB.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition CC.
In one embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition DD.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition EE.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition FF.
In one embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition GG.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition HH.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition II.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition JJ.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition KK.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition LL.
In another embodiment, the composition provides more cyclosporin A to the cornea of a person than Composition MM.
In one embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition AA.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition BB.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition CC.
In one embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition DD.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition EE.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition FF.
In one embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition GG.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition HH.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition II.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition JJ.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition KK.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition LL.
In another embodiment, the composition provides more cyclosporin A to the conjunctiva of a person than Composition MM.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 500 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, wherein topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 1000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 1400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, wherein topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 17000 ng of cyclosporin A per gram of cornea of said rabbit over a period of 24 hours after said topical administration.
In another embodiment, said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 μL drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit as determined by:
    • topically administering said composition to each eye of each of 15 female New Zealand white rabbit test subjects; and
    • determining the amount of cyclosporin A in the corneas of three subjects at times of about 0.5 hours, about 2 hours, about 6 hours, about 12 hours, and about 24 after administration to said subject;
      wherein the amount of cyclosporin A in the cornea is determined only once for each subject.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 30000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 45000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 95000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 155000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the conjunctivas of said rabbit at least about 6000 ng of cyclosporin A per gram of conjunctiva of said rabbit over a period of 24 hours after said topical administration.
In another embodiment, said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 μL drop of said composition to each eye of a New Zealand rabbit provides at least about 6000 ng of cyclosporin A per gram of conjunctiva to the conjunctivas of said rabbit as determined by:
    • topically administering said composition to each eye of each of 15 female New Zealand white rabbit test subjects; and
    • determining the amount of cyclosporin A in the conjunctivas of three subjects at times of about 0.5 hours, about 2 hours, about 6 hours, about 12 hours, and about 24 after administration to said subject;
      wherein the amount of cyclosporin A in the conjunctiva is determined only a single time for each subject.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 5000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 7000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 10000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit.
In another embodiment said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of conjunctiva to the conjunctiva of said rabbit. In another embodiment, the blood level of cyclosporin A is less than 0.1 mg/mL for a person for whom the composition has been administered twice a day topically to both eyes in 35 microliter drops for twelve months.
Pharmacokinetic Study 1
A 35 μL aliquot of one of three test formulations was topically administered to each eye of a female New Zealand White rabbit (n=3 rabbits/time point). At 0.5, 2, 6, 12, 24, 48 and 144 hours post-dose, cornea, conjunctiva, sclera, eyelid margin, nasolacrimal duct, and blood samples were collected. Samples collected from naïve rabbits (n=2) served as pre-dose samples. The quantitation ranges were 0.2-40 ng/mL in blood, 0.1-200 ng in cornea and conjunctiva, 0.1-100 ng in eyelid margin and nasolacrimal duct, and 0.1-20 ng in sclera and lacrimal gland.
The pharmacokinetic parameters of cyclosporine A in ocular tissues following a single ophthalmic instillation of one of three 0.05% cyclosporine A formulations are summarized in Table 1 below:
TABLE 1
Composition F Composition E Compositon D
Cmax AUC0-t t1/2 Cmax AUC0-t t1/2 Cmax AUC0-t t1/2
Tissue/Matrix (ng/g) (ng · hr/g) (hr) (ng/g) (ng · hr/g) (hr) (ng/g) (ng · hr/g) (hr)
Cornea 4050 163000 41.3 1100 76200 41.7 536 29300 49.8
Conjunctiva 4460 18100 11.3 2560 11600 5.57 694 5290 4.55
Sclera 545 6110 29.7 136 2840 24.8 53.0 1040 18.7
Eyelid Margin 3120 38300 42.5 2020 42200 38.1 2450 27700 24.4
Nasolacrimal 195 2190 NC 74.4 1190 NC 72.0 279 NC
Duct
Blood 2.21 NC NC 0.441 NC NC BLQ BLQ NC
NC = Not calculable
BLQ = Below the limit of quantitation

Briefly summarizing, following a single ocular instillation of a 0.05% cyclosporine A formulation, the highest cyclosporine A ocular tissue exposure levels were observed from Composition F, followed by the Composition E, followed by Composition D.
Materials
Test Articles
Compositions D, E, and F, as described above, were used for these experiments.
Chemicals, Reagents and Supplies
All other chemicals were reagent grade or better.
Animals
Species, Strain, Sex, Age, Size, Source, and Identification
Female New Zealand White rabbits weighing 1.8 to 2.6 kg were purchased from Charles River (St. Constant, Quebec, Canada). A permanent ear tag was used to identify animals.
Justification
Similarities between the ocular anatomies of rabbits and humans make the rabbit an attractive animal model.
Animal Husbandry
All animals were housed in environmentally-controlled facility with a time-controlled fluorescent lighting system providing a daily 12-hour light/12-hour dark period. Room temperature was maintained between 61 and 72° F., and relative humidity between 30 and 70%. Airflow ranged from 10 to 30 air changes per hour. Temperature, humidity, and airflow were monitored by the Edstrom Watchdog system version 4.0.
The animals were provided Certified Hi-Fiber Rabbit Diet. Diet certification and analysis were provided by the vendor. No analysis outside those provided by the manufacturer was performed. Drinking water that was purified by a reverse osmosis process was offered ad libitum. Water was periodically analyzed for any contaminants that may interfere with the conduct of this study.
The manufacturer conducted analysis of animal feed.
Animal Acclimation
During the acclimatization period at Allergan, animals were kept under daily observation for any change in general health or behavior. Rabbits were quarantined for at least five days prior to the start of the study. All animals appeared healthy prior to and for the duration of the study.
Animal Termination and Disposal
Animals were euthanized via injection of at least 1 mL of sodium pentobarbital into a marginal ear vein.
Study Design and Experimental Procedures
Study Design
TABLE 1
Study design
Animal species and Rabbit, New Zealand White
strain
Gender Female
Number 3 rabbits/time point
2 rabbits at pre-dose (bioanalytical
controls)
Body Weights 1.8-2.8 kg
Dosing Regimen Topical ocular, single dose, bilateral
Dose Volume 35 μL
Test Article Formulations containing 0.05% AGN
192371 (cyclosporine A)
Time Points 0.5, 2, 6, 12, 24, 48, and 144 hours
post-dose
Tissues/Matrices Cornea, conjunctiva, sclera,
nasolacrimal duct, eyelid margin and
blood
Assay Method LC-MS/MS
Analyte AGN 192371 (Cyclosporine A)
Quantitation Range Blood: 0.5-40 ng/mL
Cornea: 0.1-200 ng
Conjunctiva: 0.1-200 ng
Eyelid Margin: 0.1-100 ng
Nasolacrimal Duct: 0.1-100 ng
Sclera:: 0.1-20 ng
Single bilateral dose, 3 rabbits (6 eyes and 3 blood samples) per time point. Two animals in group 4 were not dosed and were used as bioanalytical controls. Prior to dosing, 65 animals were weighed and assigned to 4 study groups. The study design is presented in Table 1. The four study groups are presented in the Table 2 below:
TABLE 2
Dose
Group Treatment (μL) Frequency n
1 Composition F 35 Single Bilateral 3F per time
Dose point
(total of 21F)
2 Composition E 35 Single Bilateral 3F per time
Dose point
(total of 21F)
3 Composition D 35 Single Bilateral 3F per time
Dose point
(total of 21F)
4 No Dose 2F
(total of 2F)
n = Number of animals per group
F = Female

Pretreatment Examinations
Prior to placement on study, a physical examination was performed on each animal. Gross observations were recorded prior to drug administration and immediately after ocular dose using a standardized data collection sheet.
Randomization
Prior to dosing, 65 animals were weighed and randomly assigned to four study groups.
Dosing Procedure:
Animals were dosed once by ocular instillation bilaterally at Hour 0 of the study. Immediately prior to dosing, the eye was inspected for any abnormalities, such as infection, red eye, or visible damage. Only animals without visible abnormalities were used. The lower eyelid was gently pulled out and away from the eye. Using a Gilson precision pipette, 35 μL of dosing solution was instilled into the lower cul-de-sac of each eye. The time of dose administration was recorded. The eye was gently held closed for approximately 5 seconds to ensure even dose distribution around the eye. Gross ocular observations were performed following dosing. The animal, including the dosed eyes, were subjectively evaluated for signs of irritation. Observations were recorded.
Mortality/Morbidity
Animals were observed for mortality/morbidity during the study.
Body Weights
Animals were weighed the day before dose administration and subsequently randomized.
Pre-Necropsy Blood Collection
Blood was collected from each rabbit prior to euthanasia/necropsy. Animals were anesthetized with an intravenous injection of a ketamine/xylazine cocktail (87 mg/mL ketamine, 13 mg/mL xylazine) at a volume of 0.1 mL/kg. Blood was collected via cardiac puncture. Approximately 5 mL of blood was collected into 10 mL lavender top (K3 EDTA) tubes. Blood samples were stored at or below approximately −15° C. until bioanalysis.
Euthanasia
Animals were euthanized with an intravenous injection of commercial euthanasia solution following blood collection.
Necropsy and Collection of Ocular Tissues
Ocular samples were collected from both eyes, blotted dry where applicable, weighed and placed in separate, appropriately labeled, silanized vials, at the time of necropsy. Both eyes were rinsed with LENS PLUS® in order to clear residual surface formulation remaining on the ocular surface.
Conjunctiva
The upper and lower conjunctiva from each eye were removed and pooled, weight recorded, placed into separate screw-cap glass 13×100 silanized test tubes and immediately placed on ice. Samples were stored at or below −15° C. until bioanalysis.
Cornea
The entire cornea was removed from each eye; weight recorded, placed into separate screw-cap glass 13×100 silanized test tubes and immediately placed on ice. Samples were stored at or below −15° C. until bioanalysis.
Sclera
The sclera was removed from each eye; weight recorded, placed into separate screw-cap glass 13×100 silanized test tubes and immediately placed on ice. Samples were stored at or below −15° C. until bioanalysis.
Nasolacrimal Duct
Tissue containing the nasolacrimal duct associated with each eye was removed; weight recorded, placed into screw-cap glass 13×100 silanized test tubes and immediately placed on ice. Samples were stored at or below −15° C. until bioanalysis.
Eyelid Margin
The eyelid margins were removed from each eye; weight recorded, placed into separate screw-cap glass 13×100 silanized test tubes and immediately placed on ice. Samples were stored at or below −15° C. until bioanalysis.
Sample Storage
Blood and ocular tissue samples were stored at or below −15° C. until bioanalysis.
Bioanalysis
Ocular tissue and blood concentrations were quantified using the following method.
Ocular tissue samples were extracted by soaking over night with 2.0 mL methanol at 4° C. This was followed by a second soak with 2.0 mL methanol and shaking for approximately one hour at room temperature. An aliquot of 1 mL from a total of 4 mL organic extract was removed (all 4 mL were analyzed for lacrimal gland samples), and internal standard added (20 μL of 500 ng/mL of CsG). The methanolic extract was evaporated to dryness and reconstituted with 200 μL of 2 mM ammonium acetate/0.4% formic acid in 50:50 acetonitrile:water for LC MS/MS analysis. The bioanalytical procedure for analysis of blood samples involved addition of internal standard, CsG (10 μL of 500 ng/mL) to 0.5 mL aliquots of K3 EDTA-treated rabbit blood.
Following incubation of blood sample for 30 minutes at 37° C., the samples were acidified with 0.1 N HCL (2 mL). Methyl t-butyl ether (4 mL) was added to each sample and mixed for 15 minutes. The organic layer was removed and made basic by addition of 0.1 N NaOH (2 mL). The organic extract was separated from the aqueous layer, evaporated to dryness and reconstituted with 200 μL of 2 mM ammonium acetate/0.4% formic acid in 50:50 acetonitrile:water for LC MS/MS analysis. Aliquots (50 μL) of the reconstituted samples were analyzed by LC-MS/MS using a PE Sciex API 3000 mass spectrometer (Applied Biosystems, Foster City, Calif.), Leap autosampler (Carrboro, N.C.), and HPLC pumps (Shimadzu Scientific Instruments, Columbia, Md.). Reverse-phase HPLC was performed on a Keystone BDS C8 column (3 μm, 2.1×50 mm, 65° C.) with solvent gradient elution (A=2 mM ammonium acetate/0.4% formic acid in water and B=2 mM ammonium acetate/0.4% formic acid in acetonitrile) at a flow rate of 0.3 mL/min. The precursor-product ion pairs used in MRM analysis were: 1203 (MH)+→425.5 for CsA and m/z 1217 (MH)+→425.5 for IS(Cyclosporin G). The total analysis time was 5 min, with retention times of CsA and CsG at approximately 1.82 and 1.86 minutes, respectively.
Data Treatment
Data Collection
Pre and post treatment gross ocular examinations
Body Weights: Randomization at Day −1
Dosing Notes
Mortality/Morbidity
Blood Samples: Pre-necropsy
Ocular Tissue Samples: Post-necropsy
Data Calculation and Outlier Analysis
All data was used in calculations unless omitted for reasons justified in the raw data.
Pharmacokinetic Analysis
Thermo Electron Watson™ (Philadelphia, Pa.) and Microsoft® Excel (Redmond, Wash.) were used for pharmacokinetic calculations. The pharmacokinetic parameters listed below were calculated using a known non-compartmental approach (see Tang-Lui, et. al. Pharmaceutical Research, Vol 5, No. 4, 1988, 238-241). The pharmacokinetic data was described using descriptive statistics such as mean and standard deviation whenever possible. Area under the concentration-time profile (AUC) values were reported as a composite AUC and whenever possible, ±standard error of the mean (SEM).
PK Parameter Description
Cmax (ng/mL) or Maximum observed concentration
(ng/g)
Tmax (hr) Time corresponding to maximum observed
concentration
AUC0-t (ng · hr/g) Area under concentration time curve from time zero
to the last quantifiable time point using the
random method for non-sequential sampling
t1/2 (hr) Half-life
MRT (hr) Mean residence time

Values Below the Limit of Quantitation and Number Rounding
If more than half of the concentration values contributing to a calculation of the mean were below limit of quantitation (BLQ), then the statistics were reported as non-calculable (NC). If half or more of the values were quantifiable, then any BLQ values were replaced with a value of “0”, and the mean and its standard deviation (SD) were calculated with these replaced values. The mean and standard deviation of the mean were calculated at each sampling time point within each treatment group. Whenever the sample size was less than or equal to 2, only mean values were listed. All mean values were reported to 3 significant figures and standard deviations were reported to the same decimal place as their respective mean values.
Protocol Deviations
    • Prior to collection of ocular tissue samples at the 6 hour time point, the eyes were not rinsed with Lens Plus® to clear any residual surface formulation remaining on the ocular surface. It is believed that this deviation will have minimal impact on the results derived from this study since in general this drug is rapidly absorbed from the ocular surface. In addition, blinking by the rabbits over 6 hours should also act to clear any residual surface formulation.
    • Abbreviations
ACN Acetonitrile
ALQ Above Limits of Quantitation
AUC Area Under the Plasma or Blood
Drug Concentration - Time Curve
AUCExtrap Extrapolated Area Under the
Plasma or Blood Drug
Concentration Time Curve from
Time 0 to the Last Quantifiable
Timepoint
BID Two Times Daily
BLQ Below Limit of Quantitation
BMS Bioanalytical Mass Spectrometry
CFR Code of Federal Regulations
C0 or C0 Extrapolated Plasma or Blood
Drug Concentrations at the Time 0
Cmax or Cmax Maximal Drug Concentration
CONC Concentration
DG Day of Gestation
DSE Drug Safety Evaluation
EDTA(K3) Potassium
Ethylenediaminetetraacetic Acid
F Female
GD Gestation Day
FDA United States Food and Drug
Administration
GLP Good Laboratory Practice
IC Intracardiac
IS Insufficient Sample Received
IM Intramuscular
IU International Units
IV Intravenous
IVT Intravitreal
LC-MS/MS Liquid Chromatography Tandem
Mass Spectrometry
LLOQ Lower Limit of
Quantitation
M Male
N, n, No., no. Number
N/A, N.A., or Not Applicable
n/a
N/C, N.C., NC, Not Calculable
or n/c
NR No Result/Not Reported
NS No Sample
NZW New Zealand White
OD Right Eye
OU Both Eyes
PKDM Pharmacokinetics and Drug
Metabolism
PO By Mouth
QID Four Times Daily
QNS Quantity Not Sufficient
SD, S.D., or Standard Deviation
sd
SE Standard Error
Sec Seconds
SMP Sample
T½ or T1/2 Drug Half Life
TA Triamcinolone Acetonide
TID Three Times Daily
TK Toxicokinetic
Tmax or Tmax Time at which Cmax is
Observed
U Units
ULOQ Upper Limit of
Quantitation
Note:
Not all abbreviations listed may appear in this report.

Results and Discussion
Cornea
The mean concentrations and pharmacokinetic parameters are summarized in Tables 3 and 4. The concentration-time profiles of cyclosporine A in cornea following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 1.
TABLE 3
Mean cornea concentrations of cyclosporine A following a single
bilateral topical ocular instillation of one of three 0.05% cyclosporine
A formulations to New Zealand White rabbits.
Cyclosporine A concentration (ng/g)
Composition Composition Composition
Time F E D
(hr) Mean SD Mean SD Mean SD
0.5 4050 1220 1020 330 295 201
2 2740 620 1100 190 432 142
6 3030 750 1010 170 536 138
12 2530 430  858 267 417 127
24  1570a 390   891a 115  256a 28.2
48  1240a 230   622a 118  238a 76.6
144   222a 61   125a 47    52.5a 13.2
Mean values represent an average of n = 6
aConcentration time points used to calculate t1/2
TABLE 4
Pharmacokinetic parameters in cornea of cyclosporine
A following a single bilateral topical ocular
instillation of one of three 0.05% cyclosporine A
formulations to New Zealand White rabbits.
Parameter Composition F Composition E Composition D
Cmax (ng/g)  4050 ± 1220 1100 ± 190  536 ± 138
Tmax (hr) 0.500 2.00 6.00
AUC0-t 163000 ± 7000 76200 ± 3300 29300 ± 2000
(ng · hr/g)a
AUC0-24 59000 22100 9450
(ng · hr/g)
t1/2 (hr) 41.3 42.2 49.8
MRT (hr) 50.3 56.5 61.6
aAn AUC interval of 0-144 hours was used for calculations for the three formulations

Composition F
Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the cornea with a peak corneal concentration (Cmax) of 4050±1220 ng/g, occurring 0.500 hours post-dose. The area under the concentration-time curve (AUC0-t) value through the last quantifiable time point was 163000±7000 ng·hr/g and the AUC0-24 value was 59000 ng·hr/g. The terminal half-life (t1/2) was 41.3 hours and the mean residence time (MRT) was 50.3 hours.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A was absorbed into the cornea with Cmax value of 1100±190 ng/g, occurring 2.00 hours post-dose. The AUC0-t value was 76200±3300 ng·hr/g and the AUC0-24 value was 22100 ng·hr/g. The terminal t1/2 was 41.7 hours and the MRT was 56.5 hours.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A was absorbed into the cornea with a Cmax value of 536±138 ng/g, occurring 6.00 hours post-dose. The AUC0-t value was 29300±2000 ng·hr/g and the AUC0-24 value was 9450 ng·hr/g. The terminal t1/2 was 49.8 hours and the MRT was 61.6 hours.
Conjunctiva
The mean concentrations and pharmacokinetic parameters are summarized in Tables 5 and 6. The concentration-time profiles of cyclosporine A in conjunctiva following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 2.
TABLE 5
Mean conjunctiva concentrations of cyclosporine A
following a single bilateral topical ocular
instillation of one of three 0.05% cyclosporine A
formulations to New Zealand White rabbits.
Cyclosporine A concentration (ng/g)
Time Composition F Composition E Composition D
(hr) Mean SD Mean SD Mean SD
0.5 4460 650 2560 1070 694 410
2 2170 530 1410 330 665 266
6  739 208   630a 197  330a 143
12   292a 97   178a 34  110a 52.3
24     58.2a    12.5     60.5a 32.5    20.5a 13.2
48     26.9a 19.1 BLQ BLQ
144 BLQ BLQ BLQ
Mean values represent an average of n = 6
BLQ = Below the limit of quantitation
aConcentration time points used to calculate t1/2
TABLE 6
Pharmacokinetic parameters in conjunctiva of cyclosporine
A following a single bilateral topical ocular instillation of
one of three 0.05% cyclosporine A formulations to
New Zealand White rabbits.
Parameter Composition F Composition E Composition D
Cmax (ng/g) 4460 ± 650 2560 ± 1070 694 ± 410
Tmax (hr) 0.500 0.500 0.500
AUC0-t 18100 ± 800a  11600 ± 700b 5290 ± 480b 
(ng · hr/g)
AUC0-24 17100 11600 5290
(ng · hr/g)
t1/2 (hr) 11.3 5.57 4.55
MRT (hr) 7.37 5.93 6.07
aAn AUC interval of 0-48 hours was used for calculations
bAn AUC interval of 0-24 hours was used for calculations

Composition F
Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the conjunctiva with a Cmax value of 4460±650 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 18100±800 ng·hr/g and the AUC0-24 value was 17100 ng·hr/g. The terminal t1/2 was 11.3 hours and the MRT was 7.37 hours.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the conjunctiva with a Cmax value of 2560±1070 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 11600±700 ng·hr/g. The terminal t1/2 was 5.57 hours and the MRT was 5.93 hours.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A was rapidly absorbed into the conjunctiva with a Cmax value of 694±410 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 5290±480 ng·hr/g. The terminal t1/2 was 4.55 hours and the MRT was 6.07 hours.
Sclera
The mean concentrations and pharmacokinetic parameters are summarized in Tables 7 and 8. The concentration-time profiles of cyclosporine A in sclera following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 3.
TABLE 7
Mean sclera concentrations of cyclosporine A
following a single bilateral topical ocular
instillation of one of three 0.05% cyclosporine A
formulations to New Zealand White rabbits.
Cyclosporine A concentration (ng/g)
Time Composition F Composition E Composition D
(hr) Mean SD Mean SD Mean SD
0.5 545 98 136 44 52.5 29.3
2 294 74 120 34 49.4 24.5
6 210 58 83.7 14.0 53.0 10.9
12 133 25 51.0 19.1 28.6a 3.7
24 51.4a 9.4 36.5a 9.9 13.5a 2.3
48 24.2a 7.1 13.0a 3.61 7.10a 3.09
144 2.92a 0.40 1.14a 1.27 BLQ
Mean values represent an average of n = 6
BLQ = Below the limit of quantitation
aConcentration time points used to calculate t1/2
TABLE 8
Pharmacokinetic parameters in sclera of cyclosporine
A following a single bilateral topical ocular
instillation of one of three 0.05% cyclosporine A
formulations to New Zealand White rabbits.
Parameter Composition F Composition E Composition D
Cmax (ng/g) 545 ± 98 136 ± 43 53.0 ± 10.9
Tmax (hr) 0.500 0.500 6.00
AUC0-t 6110 ± 260a 2840 ± 150a 1040 ± 50b
(ng · hr/g)
AUC0-24 3900 1560 792
(ng · hr/g)
t1/2 (hr) 29.7 24.8 18.7
MRT (hr) 25.3 26.9 23.8
aAn AUC interval of 0-144 hours was used for calculations
bAn AUC interval of 0-48 hours was used for calculations
Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the sclera with a Cmax value of 545±98 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 6110±260 ng·hr/g and the AUC0-24 value was 3900 ng·hr/g. The terminal t1/2 was 29.7 hours and the MRT was 25.3 hours.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the sclera with a Cmax value of 136±43 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 2840±150 ng·hr/g and the AUC0-24 value was 1560 ng·hr/g. The terminal t1/2 was 24.8 hours and the MRT was 26.7 hours.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A was absorbed into the sclera with a Cmax value of 53.0±10.9 ng/g, occurring 6.00 hours post-dose. The AUC0-t value was 1040±50 ng·hr/g and the AUC0-24 value was 792 ng·hr/g. The terminal t1/2 was 18.7 hours and the MRT was 23.8 hours.
Eyelid Margin
The mean concentrations and pharmacokinetic parameters are summarized in Tables 9 and 10. The concentration-time profiles of cyclosporine A in the eyelid margin following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 4.
TABLE 9
Mean eyelid margin concentrations of cyclosporine A
following a single bilateral topical ocular instillation of one of
three 0.05% cyclosporine A formulations to New Zealand White
rabbits.
Cyclosporine A concentration (ng/g)
Time Composition F Composition E Composition D
(hr) Mean SD Mean SD Mean SD
0.5 3120  1040 2020  980 1800  900
2 1710  300 1380  630 2450  970
6 679 135 547 300 430 214
12 787 280 910 199 662 506
24  263a 158  138a 87  222a 172
48  223a 207  362a 437  112a 82
144    40.0a 22.5   24.9a 23.4     7.30a 12.64
Mean values represent an average of n = 6
aConcentration time points used to calculate t1/2
TABLE 10
Pharmacokinetic parameters in eyelid margin of
cyclosporine A following a single bilateral topical
ocular instillation of one of three 0.05% cyclosporine
A formulations to New Zealand White rabbits.
Parameter Composition F Composition E Composition D
Cmax (ng/g)  3120 ± 1040 2020 ± 980  2450 ± 970
Tmax (hr) 0.500 0.500 2.00
AUC0-t 38300 ± 5300 42200 ± 10800 27700 ± 3300
(ng · hr/g)a
AUC0-24 19900 17600 18000
(ng · hr/g)
t1/2 (hr) 42.5 38.2 24.4
MRT (hr) 40.5 38.4 21.9
aAn AUC interval of 0-144 hours was used for calculations for the three formulations

Composition F
Following a single bilateral ocular instillation of Composition F, cyclosporine A was rapidly absorbed into the eyelid margin with a Cmax value of 3120±1040 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 38300±5300 ng·hr/g and the AUC0-24 value was 19900 ng·hr/g. The terminal t1/2 was 42.5 hours and the MRT was 40.5 hours.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A was rapidly absorbed into the eyelid margin with a Cmax value of 2020±980 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 42200±10800 ng·hr/g and the AUC0-24 value was 17600 ng·hr/g. The terminal t1/2 was 38.1 hours and the MRT was 38.4 hours.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A was absorbed into the eyelid margin with a Cmax value of 2450±970 ng/g, occurring 2.00 hours post-dose. The AUC0-t value was 27700±3300 ng·hr/g and the AUC0-24 value was 18000 ng·hr/g. The terminal t1/2 was 24.4 hours and the MRT was 21.9 hours.
Nasolacrimal Duct
The mean concentrations and pharmacokinetic parameters are summarized in Tables 11 and 12. The concentration-time profiles of cyclosporine A in nasolacrimal duct tissue following a single bilateral ocular administration of one of three 0.05% cyclosporine A formulations to rabbits are presented in FIG. 5.
TABLE 11
Mean nasolacrimal duct concentrations of
cyclosporine A following a single bilateral topical
ocular instillation of one of three 0.05%
cyclosporine A formulations to New Zealand White
rabbits.
Cyclosporine A concentration (ng/g)
Time Composition F Composition E Composition D
(hr) Mean SD Mean SD Mean SD
0.5 194 201 74.4 20.9 72.0 91.7
2 43.7 44.1 37.2 43.6 37.4 13.8
6 18.2 15.2 BLQ 11.8 10.0
12 24.2 12.0 35.5 21.5 14.9 8.4
24 BLQ BLQ BLQ
48 BLQ 4.68 5.15 BLQ
144 1.71 1.93 BLQ BLQ
Mean values represent an average of n = 6
BLQ = Below the limit of quantitation
TABLE 12
Pharmacokinetic parameters in nasolacrimal duct of
Cyclosporine A following a single bilateral topical
ocular instillation of one of three 0.05%
cyclosporine A formulations to New Zealand White rabbits.
Parameter Composition F Composition E Composition D
Cmax (ng/g)  195 ± 201 74.4 ± 20.9 72.0 ± 91.7
Tmax (hr) 0.500 0.500 0.500
AUC0-t   2190 ± 350a 1190 ± 212b  279 ± 39c 
(ng · hr/g)
AUC0-12 478 ± 86 465 ± 106 279 ± 39 
(ng · hr/g)
t1/2 (hr) NC NC NC
MRT (hr)d 17.6   24.7   12.1  
NC = Not calculable
aAn AUC interval of 0-144 hours was used for calculations
bAn AUC interval of 0-48 hours was used for calculations
cAn AUC interval of 0-12 hours was used for calculations
dA time interval of 0-12 hours was used for calculations

Composition F
Following a single bilateral ocular instillation of Composition F, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a Cmax value of 195±201 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 2190±350 ng·hr/g and the AUC0-12 value was 478±86 ng·hr/g. The MRT was 17.6 hours.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a Cmax value of 74.4±20.9 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 1190±210 ng·hr/g and the AUC0-12 value was 465±106 ng·hr/g. The MRT was 24.7 hours.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A rapidly drained into and was then absorbed into the nasolacrimal duct tissue with a Cmax value of 72.0±91.7 ng/g, occurring 0.500 hours post-dose. The AUC0-t value was 279±39 ng·hr/g. The MRT was 12.1 hours.
Blood
The mean concentrations of cyclosporine A in blood are summarized in Table 13.
TABLE 13
Mean blood concentrations of Cyclosporine A following a single
bilateral topical ocular instillation of one of three 0.05%
cyclosporine A formulations to New Zealand White rabbits.
Cyclosporine A concentration (ng/mL)
Time Composition F Composition E Composition D
(hr) Mean SD Mean SD Mean SD
0.5 2.21 0.33 0.441 0.126 BLQ
2 0.463 0.021 BLQ BLQ
6 BLQ BLQ BLQ
12 BLQ BLQ BLQ
24 BLQ BLQ BLQ
48 BLQ BLQ BLQ
144 BLQ BLQ BLQ
Mean values represent an average of n = 3
BLQ = Below the limit of quantitation

Composition F
Following a single bilateral ocular instillation of Composition F, cyclosporine A was detected at 0.5 and 2 hours post-dose in the blood at concentrations of 2.21±0.33 ng/mL and 0.463±0.021 ng/mL, respectively. Cyclosporine A levels were below the limit of quantitation at all subsequent time points.
Composition E
Following a single bilateral ocular instillation of Composition E, cyclosporine A was detected at 0.5 hours post-dose in the blood at a concentration of 0.441±0.126 ng/mL. Cyclosporine A levels were below the limit of quantitation at all subsequent time points.
Composition D
Following a single bilateral ocular instillation of Composition D, cyclosporine A levels were below the limit of quantitation at all time points.
Administration of Composition F to rabbits generally delivered the highest levels of cyclosporine A to ocular tissues, on average a 5-fold increase in area under the concentration-time profile (AUC) was observed when compared to Composition D. Administration of Composition E to rabbits resulted on average in a 2-fold increase in AUC when compared to Composition D. The pharmacokinetic profile observed following Composition D administration to New Zealand White rabbits in this study was in good agreement with previously reported data.
In general, the terminal half-life and mean residence time observed were greatest for Composition F, followed by the Composition E, followed by Composition D. Thus, AUC values were reported to the last quantifiable time point, in addition to AUC through 24 hours for cornea, conjunctiva, sclera and eyelid margin and AUC through 12 hours for nasolacrimal duct to make an assessment over the same interval as to the drug levels achieved following once a day dosing. Overall, the trends observed when comparing AUC0-t values were consistent with the trends observed when comparing AUC0-24 or AUC0-12.
In conclusion, following a single ocular instillation of a 0.05% cyclosporine A formulation, the highest cyclosporine A ocular tissue exposure levels were observed when drug was formulated as an aqueous Composition F, followed by the Composition E followed by Composition D. A concomitant trend was observed in blood drug exposure.
While not intending to limit the scope of the invention, it is believed that these pharmacokinetic results suggest that significantly lower concentrations of cyclosporin A may be used in topical ophthalmic compositions than previously known and still achieve a therapeutically effective amount cyclosporin A.
Pharmacokinetic Study 2
The compositions below were prepared in an analogous manner to compositions D, E, and F.
Formulations
Composition G Composition H Composition
Aqueous Aqueous D
Ingredients Solution Solution Emulsion
Cyclosporine A 0.020 0.030 0.050
Purite 0.01% 0.01% 0.0%
(100 ppm) (100 ppm) (0 ppm)
Polysorbate 80 1.0 1.0 1.0
Glycerin 1.0 1.0 2.2
Mannitol 0.5 0.5 N/A
Sodium 0.5 0.5 N/A
Carboxymethylcellulose
(CMC) - 7LFPH
Sodium Citrate 0.4 0.4 N/A
Dihydrate
Boric Acid 0.25 0.25 N/A
Sodium Borate 0.41 0.41 N/A
Decahydrate
Potassium Chloride 0.14 0.14 N/A
Castor Oil N/A N/A 1.25
Pemulen TR-2 N/A N/A 0.05
Sodium Hydroxide N/A N/A pH 7.4
Purified Water QS QS N/A
A pharmacokinetic study was carried out using similar analytical methods to those already described. The parameters are shown below.
Test Formulations: G, H, and D
Animal species/strain: Rabbit NZW
Gender: Female
Number: 2 rabbits/timepoint (2 rabbits
blanks)
Dosing Route: Topical ocular
Dosing Regimen: Bilateral, QD(Aqueous)/BID
(Composition D) - 5 days
Dose Volume: 35 μL
Time points: Day 1 and Day 5 - 0.5, 2, 6, 12, 24 hr
post dose
Assay Method: LC-MS/MS
Analyte: Cyclosporine A
Data Analysis: Cmax, AUC0-24, AUC dose normalized
The results in cornea, tear, and blood are shown in the tables below.
TABLE 14
Cyclosporin bioavailability in the cornea.
Composition D
Composition G Composition H Emulsion, BID
Day
1 Day 5 Day 1 Day 5 Day 1 Day 5
Cmax  810 ± 530 2570 ± 650 1420 ± 930 3020 ± 440  583 ± 209 1670 ± 170
(ng/g)
AUC0-24 14700 ± 2500 33900 ± 2200 22100 ± 2800 48800 ± 3900 12100 ± 700  27900 ± 1000
(ng · hr/g)
AUC/Dose 2.12 4.93 2.12 4.71 0.349 0.807
(ng · hr/g/ng)
Total 7000 7000 10500 10500 35000 35000
Dose/24 hr
(ng)
TABLE 15
Cyclosporin bioavailability in the blood.
Restasis ®
0.02% CsA 0.03% CsA (0.05%)
Aqueous, QD Aqueous, QD Emulsion, BID
Day
1 Day 5 Day 1 Day 5 Day 1 Day 5
C0.5 hr 0.741 0.883 0.727 0.604 BLQ BLQ
(ng/mL)
n = 2 rabbits/timepoint
BLQ—Below the limit of detection (0.2 ng/mL)
TABLE 16
Cyclosporin bioavailability in the tears.
Restasis ®
0.02% CsA 0.03% CsA (0.05%)
Aqueous, QD Aqueous, QD Emulsion, BID
Day
1 Day 5 Day 1 Day 5 Day 1 Day 5
Cmax 18.2 ± 6.3 50.1 ± 29.2 31.4 ± 45.2 39.4 ± 9.7  44.2 ± 18.4 83.5 ± 33.2
(ng/mL)
AUC0-24 109 ± 15 371 ± 62  327 ± 121 397 ± 127 368 ± 51  663 ± 110
(ng · hr/mL)

Standard Compositions
These compositions (AA-MM) are particularly contemplated for use as standards for comparison for characterization of the compositions disclosed herein.
The following compositions are intended to mean those identical to those disclosed in Kanai et. al., Transplantation Proceedings, Vol 21, No 1 (February), 1989: 3150-3152, which is incorporated by reference herein:
    • Composition AA: a solution consisting of 0.025% cyclosporin A, 40 mg/mL alpha cyclodextrin, and water;
    • Composition BB: a solution consisting of 0.009% cyclosporin A, 20 mg/mL alpha cyclodextrin, and water; and
    • Composition CC: a solution consisting of 0.003% cyclosporin A, 10 mg/mL alpha cyclodextrin, and water.
The following composition is intended to mean those identical to that disclosed in Cheeks et. al., Current Eye Research, Vol 11, No 7 (1992), 641-649, which is incorporated by reference herein:
    • Composition DD: an alpha cyclodextrin solution at 40 mg/mL containing 0.025% cyclosporin A.
The following composition is intended to mean that identical that disclosed in Tamilvanan, Stp Pharma Sci November-December; 11(6):421-426, which is incorporated by reference herein, except that the concentration of cyclosporin A is different.
    • Composition EE: an emulsion consisting of cyclosporin A (0.05 w/w %), castor oil (2.5 w/w %), stearylamine (0.12 w/w %), α-tocopherol (0.01 w/w %), benzalkonium chloride (0.01 w/w %) and water up to 100 w/w %.
The following compositions are intended to mean those identical to Samples C-E disclosed in U.S. Pat. No. 5,051,402 (column 7). The entire disclosure is incorporated herein by reference.
    • Composition FF: 0.25 mL/mL of cyclosporin A, 40 mg/mL of α-cyclodextrin, and 7.79 mg/mL of sodium chloride;
    • Composition GG: 0.10 mL/mL of cyclosporin A, 20 mg/mL of α-cyclodextrin, and 8.40 mg/mL of sodium chloride; and
    • Composition HH: 0.05 mL/mL of cyclosporin A, 10 mg/mL of α-cyclodextrin, and 8.70 mg/mL of sodium chloride.
The following composition is intended to mean that identical that disclosed in Abdulrizak, Stp Pharma Sci November-December; 11(6):427-432, which is incorporated by reference herein, except that the concentration of cyclosporin A is different.
    • Composition II: an emulsion consisting of cyclosporin A (0.05 w/w %), castor oil (2.5 w/w %), Poloxamer 188, (0.425 w/w %), glycerol (2.25 w/w %), Lipoid E-80 (0.5 w/w %), stearylamine (0.12 w/w %), tocopherol (0.01 w/w %), benzalkonium chloride (0.01 w/w %), and water.
The following composition is intended to mean that identical to that disclosed in Kuwano Mitsuaki et al. Pharm Res 2002 August; 19(1):108-111.
    • Composition JJ: a solution consisting of cyclosporine A (0.0865%), ethanol (0.1%), MYS-40 (2%), HPMC (0.3 w/v %), sodium dihydrogen phosphate (0.2 w/v %), and disodium EDTA (0.01% w/v %), sodium chloride to adjust the tonicity to 287 mOsm, and water.
    • Composition KK is intended to mean that disclosed in US20010041671, incorporated by reference herein, as Formulation 1, on Table 1. Composition LL is that disclosed in US20010041671 as Formulation 3, except that the concentration of cyclosporine is reduced.
    • Composition KK: cyclosporine A (0.02%), sodium hyaluronate (0.05%), Tween 80 (0.05%), Na2HPO4.12H2O (0.08%), sorbitol (5.46%), purified water added to 100 mL, pH 7.0-7.4, and mosm/L=295-305.
    • Composition LL: cyclosporine A (0.2%), sodium hyaluronate (0.10%), Tween 80 (5.00%), Na2HPO4.12H2O (0.08%), sorbitol (5.16%), purified water added to 100 mL, pH 7.0-7.4, and mosm/L=295-305.
The following composition is intended to mean that disclosed in Example 2 of U.S. Pat. No. 5,951,971, incorporated herein by reference.
    • Composition MM: cyclosporine A (0.025 g), polyoxyl 40 stearate (0.5 g), hydroxypropyl methylcellulose (0.2 g), butylated hydroxytoluene (0.0005 g), ethanol (0.1 g), sodium chloride (0.73 g), sodium dihydrogen phosphate (0.2 g), sodium edethate (0.1 g), sodium hydroxide to adjust pH to 6.0, and water to make 100 mL.
In another embodiment the composition provides more cyclosporin A than Composition AA provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition BB provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition CC provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition DD provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition EE provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition FF provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition GG provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition HH provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition II provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition JJ provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition KK provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition LL provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition MM provides to the cornea of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition AA provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition BB provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition CC provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition DD provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition EE provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition FF provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition GG provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition HH provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition II provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition JJ provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition KK provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition LL provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition MM provides to the conjunctiva of a female New Zealand white rabbit 30 minutes after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
Comparison of two compositions in a person or animal can be carried out by, among other means, administering the claimed composition to one eye and the second composition to the second eye.
In another embodiment the composition provides more cyclosporin A than Composition AA provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition BB provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition CC provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition DD provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition EE provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition FF provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition GG provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition HH provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition II provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition JJ provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition KK provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition LL provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition MM provides to the cornea of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition AA provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition AA, wherein the drop of said composition and the drop of Composition AA are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition BB provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition BB, wherein the drop of said composition and the drop of Composition BB are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition CC provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition CC, wherein the drop of said composition and the drop of Composition CC are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition DD provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition DD, wherein the drop of said composition and the drop of Composition DD are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition EE provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition EE, wherein the drop of said composition and the drop of Composition EE are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition FF provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition FF, wherein the drop of said composition and the drop of composition FF are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition GG provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition GG, wherein the drop of said composition and the drop of composition GG are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition HH provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition HH, wherein the drop of said composition and the drop of composition HH are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition II provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition II, wherein the drop of said composition and the drop of composition II are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition JJ provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition JJ, wherein the drop of said composition and the drop of composition JJ are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition KK provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition KK, wherein the drop of said composition and the drop of composition KK are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition LL provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition LL, wherein the drop of said composition and the drop of composition LL are the same volume.
In another embodiment the composition provides more cyclosporin A than Composition MM provides to the conjunctiva of a female New Zealand white rabbit over a period of 24 hours after topical ocular administration of one drop of said composition or Composition MM, wherein the drop of said composition and the drop of composition MM are the same volume.
In one embodiment, wherein topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 500 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2000 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 2400 ng of cyclosporin A per gram of cornea of said rabbit at 30 minutes after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the corneas of said rabbit at least about 17000 ng of cyclosporin A per gram of cornea of said rabbit over a period of 24 hours after said topical administration.
In another embodiment, topical administration of one 35 μL drop of said composition to each eye of a female New Zealand white rabbit provides to the conjunctivas of said rabbit at least about 3300 ng of cyclosporin A per gram of conjunctiva of said rabbit over a period of 24 hours after said topical administration.
In another embodiment, said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 μL drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of cornea to the corneas of said rabbit as determined by:
    • topically administering said composition to each eye of each of 15 female New Zealand white rabbit test subjects, and
    • determining the amount of cyclosporin A in the corneas of three subjects at times of about 0.5 hours, about 2 hours, about 6 hours, about 12 hours, and about 24 after administration to said subject,
      wherein the amount of cyclosporin A in the cornea is determined only once for each subject.
In another embodiment, said composition is an aqueous solution containing from 0.005% to about 0.04% cyclosporin A, wherein topical administration of one 35 μL drop of said composition to each eye of a New Zealand rabbit provides at least about 17000 ng of cyclosporin A per gram of conjunctiva to the conjunctivas of said rabbit as determined by:
    • topically administering said composition to each eye of each of 15 female New Zealand white rabbit test subjects, and
    • determining the amount of cyclosporin A in the conjunctivas of three subjects at times of about 0.5 hours, about 2 hours, about 6 hours, about 12 hours, and about 24 after administration to said subject,
      wherein the amount of cyclosporin A in the conjunctiva is determined only a single time for each subject.
As mentioned above, these compositions are suitable for use in other mammals other than rabbits, including humans. Thus, any composition in the claims or elsewhere which is characterized by in vivo rabbit bioavailability testing is contemplated for use in a person or in another mammal. Defining a composition in terms of bioavailability in rabbits should not be construed to limit a method of treatment using the composition to use on rabbits, but treatment with the composition should be construed to include treatment on humans and other mammals.
The foregoing description details specific methods and compositions that can be employed to practice the present invention, and represents the best mode contemplated. However, it is apparent for one of ordinary skill in the art that further compositions with the desired pharmacological properties can be prepared in an analogous manner. Thus, however detailed the foregoing may appear in text, it should not be construed as limiting the overall scope hereof; rather, the ambit of the present invention is to be governed only by the lawful construction of the claims.

Claims (10)

What is claimed is:
1. An aqueous solution comprising cyclosporin A at a concentration of about 0.0001% (w/v), Polysorbate 80, glycerin, mannitol, carboxymethylcellulose sodium, and water, wherein the aqueous solution contains no oil.
2. The solution of claim 1, wherein the Polysorbate 80 is at a concentration of 1% (w/v), the glycerin is at a concentration of 1% (w/v), the mannitol is at a concentration of 0.5% (w/v), and the carboxymethylcellulose sodium is at a concentration of 0.5% (w/v).
3. The solution of claim 2, further comprising sodium citrate dihydrate, potassium chloride, boric acid, and sodium borate decahydrate.
4. A method comprising topically administering a composition according to claim 1 to an eye of a mammal in need thereof to enhance or restore lacrimal gland tearing.
5. The method of claim 4, wherein said method increases tear production in a tear-deficient eye.
6. The method of claim 4, wherein said method is effective in treating keratoconjunctivitis sicca.
7. The method of claim 4, wherein said method is effective in treating dry eye disease.
8. The method of claim 4 wherein the mammal is a human patient, and wherein less than 10% of human patients suffer burning or stinging when said composition is administered only once a day for a period of three months.
9. The method of claim 4 wherein the mammal is a human patient, and wherein less than 10% of human patients suffer ocular burning when said composition is administered only once a day for a period of three months.
10. The method of claim 4 wherein the composition is administered only once a day.
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US12/035,698 US20080207495A1 (en) 2006-07-25 2008-02-22 Cyclosporin compositions for ocular rosacea treatment
US15/425,836 US20170143792A1 (en) 2006-07-25 2017-02-06 Cyclosporin compositions
US17/064,988 US20210169971A1 (en) 2006-07-25 2020-10-07 Cyclosporin compositions
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Cited By (1)

* Cited by examiner, † Cited by third party
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Families Citing this family (20)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20050059583A1 (en) 2003-09-15 2005-03-17 Allergan, Inc. Methods of providing therapeutic effects using cyclosporin components
AU2016203191B2 (en) * 2006-07-25 2018-03-01 Allergan, Inc. Cyclosporin compositions
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JP2020152674A (en) * 2019-03-20 2020-09-24 株式会社リコー Method for producing solubilized product of poorly water-soluble compound
GR1010012B (en) * 2020-05-12 2021-05-27 Φαρματεν Α.Β.Ε.Ε. Preservative free pharmaceutical composition for ophthalmic administration containing cyclosporine

Citations (22)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5051402A (en) 1987-06-04 1991-09-24 Sankyo Company, Limited Pharmaceutical composition containing cyclosporin in admixture with α-
US5294604A (en) 1989-12-20 1994-03-15 The Government Of The United States Of America As Represented By The Secretary Of The Department Of Health And Human Services Method of treating ocular diseases by periocular administration of cyclosporine A or G
US5474979A (en) * 1994-05-17 1995-12-12 Allergan, Inc. Nonirritating emulsions for sensitive tissue
US5540931A (en) 1989-03-03 1996-07-30 Charles W. Hewitt Methods for inducing site-specific immunosuppression and compositions of site specific immunosuppressants
US5565302A (en) * 1995-04-21 1996-10-15 W. R. Grace & Co.-Conn. Process for preparing photosensitive resin composition
US5951971A (en) 1992-05-13 1999-09-14 Novartis Ag Ophthalmic compositions
US6008192A (en) 1997-03-12 1999-12-28 Abbott Laboratories Hydrophilic binary systems for the administration of lipophilic compounds
US20010041671A1 (en) 2000-04-07 2001-11-15 Napoli Guido Di Ophthalmic formulations
WO2002049603A1 (en) 2000-12-20 2002-06-27 Lg Household & Health Care Ltd. Compositions for prevention and alleviation of skin wrinkles
US6562873B2 (en) * 2000-07-14 2003-05-13 Allergan, Inc. Compositions containing therapeutically active components having enhanced solubility
US6656460B2 (en) 2001-11-01 2003-12-02 Yissum Research Development Method and composition for dry eye treatment
US20040092435A1 (en) 2002-11-07 2004-05-13 Peyman Gholam A. Treatment of ocular disease
US20050059583A1 (en) * 2003-09-15 2005-03-17 Allergan, Inc. Methods of providing therapeutic effects using cyclosporin components
US20050106189A1 (en) 2001-12-14 2005-05-19 Jagotec Ag Pharmaceutical formulation comprising cyclosporin and use thereof
US20050277584A1 (en) 2004-06-09 2005-12-15 Allergan, Inc. Pharmaceutical compositions comprising cyclosporins
WO2006050837A2 (en) 2004-11-09 2006-05-18 Novagali Pharma Sa Ophthalmic emulsions containing an immunosuppressive agent
US20060148686A1 (en) 2004-12-30 2006-07-06 Bausch & Lomb Incorporated Ophthalmic compositions comprising steroid and cyclosporine for dry eye therapy
WO2007008894A2 (en) 2005-07-13 2007-01-18 Allergan, Inc. Cyclosporin compositions
WO2007011880A2 (en) 2005-07-18 2007-01-25 Minu, L.L.C. Enhanced ocular neuroprotection/neurostimulation
WO2007056457A2 (en) 2005-11-09 2007-05-18 Combinatorx, Incorporated Methods, compositions, and kits for the treatment of medical conditions
WO2008014200A2 (en) * 2006-07-25 2008-01-31 Allergan, Inc. Cyclosporin compositions
US20090131307A1 (en) * 2005-07-27 2009-05-21 Tien Walter L Pharmaceutical compositions comprising cyclosporins

Family Cites Families (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
HU205861B (en) * 1986-12-19 1992-07-28 Sandoz Ag Process for producing hydrosole of pharmaceutically effective material
JPH0558906A (en) * 1991-09-06 1993-03-09 Sankyo Co Ltd Cyclosporin eye-lotion
JP2000143542A (en) * 1998-11-10 2000-05-23 Wakamoto Pharmaceut Co Ltd O / W emulsion formulation containing sparingly soluble immunosuppressant
US20030165545A1 (en) * 2002-01-30 2003-09-04 Allergan, Inc. Ophthalmic compositions including oil-in-water emulsions, and methods for making and using same
US20050058696A1 (en) * 2003-09-12 2005-03-17 Allergan, Inc. Methods and compositions for the treatment of pain and other alpha 2 adrenergic-mediated conditions
US20050276867A1 (en) * 2004-06-09 2005-12-15 Allergan, Inc. Stabilized compositions comprising a therapeutically active agent and an oxidizing preservative

Patent Citations (27)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6953776B2 (en) 1920-04-07 2005-10-11 Laboratoire Medidom S.A. Ophthalmic formulations
US5051402A (en) 1987-06-04 1991-09-24 Sankyo Company, Limited Pharmaceutical composition containing cyclosporin in admixture with α-
US5540931A (en) 1989-03-03 1996-07-30 Charles W. Hewitt Methods for inducing site-specific immunosuppression and compositions of site specific immunosuppressants
US5294604A (en) 1989-12-20 1994-03-15 The Government Of The United States Of America As Represented By The Secretary Of The Department Of Health And Human Services Method of treating ocular diseases by periocular administration of cyclosporine A or G
US6582718B2 (en) 1992-05-13 2003-06-24 Novartis Ag Cyclosporin compositions
US5951971A (en) 1992-05-13 1999-09-14 Novartis Ag Ophthalmic compositions
US20020045601A1 (en) 1992-05-13 2002-04-18 Yoichi Kawashima Ophthalmic compositions
US5474979A (en) * 1994-05-17 1995-12-12 Allergan, Inc. Nonirritating emulsions for sensitive tissue
US5565302A (en) * 1995-04-21 1996-10-15 W. R. Grace & Co.-Conn. Process for preparing photosensitive resin composition
US6008192A (en) 1997-03-12 1999-12-28 Abbott Laboratories Hydrophilic binary systems for the administration of lipophilic compounds
US6677304B2 (en) 2000-04-07 2004-01-13 Laboratorie Medidom S.A. Ophthalmic formulations
US20040106546A1 (en) 2000-04-07 2004-06-03 Napoli Guido Di Ophthalmic formulations
US20010041671A1 (en) 2000-04-07 2001-11-15 Napoli Guido Di Ophthalmic formulations
US6562873B2 (en) * 2000-07-14 2003-05-13 Allergan, Inc. Compositions containing therapeutically active components having enhanced solubility
WO2002049603A1 (en) 2000-12-20 2002-06-27 Lg Household & Health Care Ltd. Compositions for prevention and alleviation of skin wrinkles
US6656460B2 (en) 2001-11-01 2003-12-02 Yissum Research Development Method and composition for dry eye treatment
US20050106189A1 (en) 2001-12-14 2005-05-19 Jagotec Ag Pharmaceutical formulation comprising cyclosporin and use thereof
US20040092435A1 (en) 2002-11-07 2004-05-13 Peyman Gholam A. Treatment of ocular disease
US20050059583A1 (en) * 2003-09-15 2005-03-17 Allergan, Inc. Methods of providing therapeutic effects using cyclosporin components
US20050277584A1 (en) 2004-06-09 2005-12-15 Allergan, Inc. Pharmaceutical compositions comprising cyclosporins
WO2006050837A2 (en) 2004-11-09 2006-05-18 Novagali Pharma Sa Ophthalmic emulsions containing an immunosuppressive agent
US20060148686A1 (en) 2004-12-30 2006-07-06 Bausch & Lomb Incorporated Ophthalmic compositions comprising steroid and cyclosporine for dry eye therapy
WO2007008894A2 (en) 2005-07-13 2007-01-18 Allergan, Inc. Cyclosporin compositions
WO2007011880A2 (en) 2005-07-18 2007-01-25 Minu, L.L.C. Enhanced ocular neuroprotection/neurostimulation
US20090131307A1 (en) * 2005-07-27 2009-05-21 Tien Walter L Pharmaceutical compositions comprising cyclosporins
WO2007056457A2 (en) 2005-11-09 2007-05-18 Combinatorx, Incorporated Methods, compositions, and kits for the treatment of medical conditions
WO2008014200A2 (en) * 2006-07-25 2008-01-31 Allergan, Inc. Cyclosporin compositions

Non-Patent Citations (23)

* Cited by examiner, † Cited by third party
Title
Abdulrazik, M., et al., "Ocular Delivery of Cyclosporin A II. Effect of Submicron Emulsion's Surface Charge on Ocular Distribution of Topical Cyclosporin A" STP Pharma Sciences II (6), 2001, pp. 427-432.
Acheampong, Andrew A., et al., "Distribution of Cyclosporin A in Ocular Tissues After Topical Administration to Albino Rabbits and Beagle Dogs" Current Eye Research, vol. 18, No. 2, 1999, pp. 91-103.
Acheampong, Andrew, et al., "Cyclosporine Distribution into the Conjunctiva, Cornea, Lacrimal Gland, and Systemic Blood Following Topical Dosing of Cyclosporine to Rabbit, Dog, and Human Eyes" Adv Exp Med Biol 1998; 438:1001-4.
Angelov, O., et al., "Safety Assessment of Cyclosporine Ophthalmic Emulsion in Rabbits and Dogs" AN98071079, Soc Ophthalmol Eur 1997; 25-28.
Cheeks, Lisa, et al., "Influence of Vehcile and Anterior Chamber Protein Concentration on Cyclosporine Penetration Through the Isolated Rabbit Cornea" Current Eye Research, vol. 11, No. 7, 1992, pp. 641-649.
Ding, Shulin, et al., "Cyclosporine Ophthalmic O/W EMulsion: Formulation and Emulsion Characterization" AN98040585, Pharm Res 1997; 14 (11 Suppl):S41.
Encyclopedia Britannica (retrieved from http://www.britannica.com/science/emulsion-chemistry on Oct. 5, 2015, 2 pages). *
Hiroyuki, Kawano, et al., "Effectiveness of Hydrophilic Cyclosporin Eye Drops for Penetrating Keratoplasty on Albino Rabbits" Abstract SciFinder, May 26, 2006, p. 2.
IUPAC Goldbook (retrieved from http://goldbook.iupac.org/S05746.html on Oct. 8, 2015, 1 page). *
Kanai et al ('The effect of the cornea of alpha cyclodextrin vehicle for cyclosporine eye drops' Transplantation Proceedings 1989 v21 pp. 3150-3152). *
Kanai, A., et al., "The Effect on the Cornea of Alpha Cyclodextrin Vehicle for Cyclosporin Eye Drops" Transplantation Proceedings, vol. 21, No. 1, Feb. 1989, pp. 3150-3152.
Kanpolat, Ayfer, et al., "Penetration of Cyclosporin A Into the Rabbit Cornea and Aqueous Humor After Topical Drop and COllagen Shield Administration" The CLAO Journal, Apr. 1994, vol. 20, No. 2, pp. 119-122.
Kuwano, Mitsuaki, et al., "Cyclosporine A Formulation Affects Its Ocular Distribution in Rabbits" Pharmaceutical Research, 2002, vol. 19, No. 1, pp. 108-111.
Lallemand, F., et al., "Cyclosporin A Delivery to the Eye: A Pharmaceutical Challenge" Eur J Pharm Biophann, Nov. 2003, 56 (3), pp. 307-318.
Lyons, R. T., et al., "Influence of Three Emulsion Formulation Parameters on the Ocular Bioavailability of Cyclosporine A in Albino Rabbits" Am Assoc Pharm Sci 2000;2(4):1 page.
Mizutani, Hideki, et al., "Investigation of Pharmaceutical Characteristics of Cyclosporin A Aqueous Eye Drops and Their Topical Application in Clinical Practice" JPN J. Pharm. Health Care Sci., 2005, 31(7):563-566.
Quintana-Hau, et al., "In Vitro Study of Corneal Retention of Cyclosporine-A from Different Formulations" Invest Ophthalmol Vis Sci, 2004; 45: E-Abstract 67.
Rao, S.N., "Comparison of the Efficacy of Topical Cyclosporine 0.05% Compared With Tobradex for the Treatment of Posterior Blepharitis" Invest Ophthalmol Vis Sci 2005; 46: E-Abstract 2662.
Reynolds et al, "Therapeutic option for the management of early neurotrophic keratopathy: A case report and review", Journal of the American Optometric Association, vol. 77. No. 10, pp. 503-507, 2006.
Rubin, Michael, et al., "Efficacy of Topical Cyclosporin 0.05% in the Treatment of Posterior Blepharitis" Journal of Ocular Pharmacology and Therapeutics, vol. 22, No. 1, 2006, pp. 47-53.
Small, Dave, et al., "The Ocular Pharmacokinetics of Cyclosporine in Albino Rabbits and Beagle Dogs" Assoc. Ocular Pharm Ther 1999; 54.
Tatlipinar, S., et al., "Topical Ciclosporin in the Treatment of Ocular Surface Disorders" Br J Ophthalmol, 2005, 89(10), pp. 1363-7.
Tesavibul, N., et al., "Topical Cyclosporine A (CsA) for Ocular Surface Abnormalities in Graft Versus Host Disease Patients" Invest Ophthalmol Vis Sci Feb. 1996; 37(3):S1026.

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